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Front. Cell Dev. Biol., 20 May 2021
Sec. Molecular and Cellular Oncology
This article is part of the Research Topic Tumor Micro-environment and Drug Resistance View all 33 articles

The Role of Tumor-Stroma Interactions in Drug Resistance Within Tumor Microenvironment

\r\nYanghong Ni,&#x;Yanghong Ni1,2†Xiaoting Zhou,&#x;Xiaoting Zhou1,2†Jia Yang,Jia Yang1,2Houhui Shi,Houhui Shi1,2Hongyi Li,Hongyi Li1,2Xia Zhao*Xia Zhao2*Xuelei Ma*Xuelei Ma1*
  • 1Department of Biotherapy, State Key Laboratory of Biotherapy and Cancer Center, West China Hospital, Collaborative Innovation Center of Biotherapy, Sichuan University, Chengdu, China
  • 2Department of Gynecology and Obstetrics, Development and Related Disease of Women and Children Key Laboratory of Sichuan Province, Key Laboratory of Birth Defects and Related Diseases of Women and Children, Ministry of Education, West China Second Hospital, Sichuan University, Chengdu, China

Cancer cells resistance to various therapies remains to be a key challenge nowadays. For a long time, scientists focused on tumor cells themselves for the mechanisms of acquired drug resistance. However, recent evidence showed that tumor microenvironment (TME) is essential for regulating immune escape, drug resistance, progression and metastasis of malignant cells. Reciprocal interactions between cancer cells and non-malignant cells within this milieu often reshape the TME and promote drug resistance. Therefore, advanced knowledge about these sophisticated interactions is significant for the design of effective therapeutic approaches. In this review, we highlight cancer-associated fibroblasts (CAFs), tumor-associated macrophages (TAMs), tumor-associated neutrophils (TANs), myeloid-derived suppressor cells (MDSCs), T-regulatory lymphocytes (Tregs), mesenchymal stem cells (MSCs), cancer-associated adipocytes (CAAs), and tumor endothelial cells (TECs) existing in TME, as well as their multiple cross-talk with tumor cells, which eventually endows tumor cells with therapeutic resistance.

Introduction

Over decades, cancer has always been a major public health problem worldwide. According to the statistics reported by the American Cancer Society in 2020, there are nearly 1.8 million new cancer cases and 600 thousand cancer deaths in the United States (Siegel et al., 2020). In general, antitumor treatments mainly include surgery, chemotherapy, radiotherapy, immunotherapy, hormone therapy and targeted therapy. Patients can obtain more obvious effects in the initial stage of treatment, while the emergence of drug resistance often becomes an inevitable obstacle to clinical recovery in the late stage. For a long time, scientists focused on tumor cells themselves for the mechanisms of acquired drug resistance, such as the up-regulation of drug efflux pump protein (Amawi et al., 2019), epigenetic abnormalities (Shah and Rawal, 2019), oncogenic mutations and tumor heterogeneity etc. (Hientz et al., 2017; Zhang H. et al., 2017; Vaidya et al., 2020). The concept of tumor microenvironment (TME) was first proposed by Stephen Paget who indicated that the relationship between breast cancer and its microenvironment is like “seed and soil” (Paget, 1989). TME refers to the local biological environment where tumor cells exist and the number of cancer cells varies from 5 to 100% (Ambrose et al., 2015). It is currently considered to be an acidic and hypoxic milieu infiltrated by cancer cells and accessory cells, including stromal cells, endothelial cells, immune cells, mesenchymal cells, adipocytes and pericytes, as well as extracellular matrix and cytokines (Hui and Chen, 2015; Yamaguchi and Perkins, 2018).

Tumor microenvironment serves as safeguard to tumor cells by providing mechanical support or secreting different cytokines to evade treatment (Figure 1; Kodet et al., 2018). Diverse heterogeneous cells along with their secretory cytokines constitute a complex network, which allows tumor cells to proliferate rapidly, maintain stemness, insensitive to medication and escape from immune surveillance. In fact, non-inherent-adaptive resistance, also called non-cell-autonomous resistance, is therapeutically dependent (Calcinotto et al., 2018). TME is involved in the initiation and maintenance of non-cell autonomous resistance by a variety of mechanisms, including hypoxia, low PH, shifts and polarizations in the immune cell population, vascular abnormalities and diverse stroma cells-derived secretomes, exosomes, soluble factors. In order to deeply understand progression and drug resistance of tumor cells, a thorough knowledge of the interactions between tumor cells and their microenvironment is needed. Therefore, we reviewed a series of non-malignant cells constituting the tumor microenvironment and how they interplay with tumor cells to promote therapeutic resistance with an expectance to spark new ideas of designing more specific approaches for cancer.

FIGURE 1
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Figure 1. A schematic overview of tumor microenvironments. Tumor microenvironment refers to the local biological environment where tumor cells exist, and are composed of tumor cells, stromal cells and immune cells. TME is involved in the initiation and maintenance of non-cell autonomous resistance by a variety of mechanisms, including hypoxia, low PH, shifts and polarizations in the immune cell population, vascular abnormalities and diverse stroma cells-derived secretomes, exosomes, soluble factors. TME serves as safeguard to tumor cells by providing mechanical support or secreting different cytokines to evade treatment. Treg, regulatory T lymphocytes; MSC, mesenchymal stem cells; T, T lymphocytes; B, B lymphocytes; DC, dendritic cells; N, neutrophils; M, macrophages; NK, natural killer cells; E, epithelial cells; F, fibroblasts; CAA, cancer-associated adipocytes; L, lymphatic endothelial cells; TEC, tumor endothelial cells; CSC, cancer stem cells; TAM, tumor-associated macrophages; CAF, cancer-associated fibroblasts; MDSC, myeloid-derived suppressor cells; EMT, epithelial-mesenchymal transition. The figure was created with BioRender.com.

Cancer Associated Fibroblasts (CAFs) and Drug Resistance

Cancer associated fibroblasts (CAFs) are one of the most important components of TME. Numerous researches have suggested its role in forming the communication networks with tumor cells and other elements in TME, which is responsible for therapeutic resistance in pancreatic cancer, colorectal neoplasm, breast cancer, ovarian neoplasm, lung cancer, gastric cancer and so on (Mao et al., 2015; Zhou B. et al., 2016; Wen et al., 2017; Cazet et al., 2018; Tang et al., 2018; Wei et al., 2018; Yi et al., 2018; Hu et al., 2019; Wang L. et al., 2019). The origins of CAFs are diverse. In addition to the normal activated fibroblasts, marked by the expression of α-smooth muscle actin (α-SMA), CAFs can also evolve from other cell types, such as bone marrow-derived cells (BMDCs) (Mishra et al., 2008), epithelial cells undergone epithelial-mesenchymal transition (EMT) (Kalluri and Neilson, 2003), endothelial cells following endothelial-to-mesenchymal transition (EndMT) (Zeisberg et al., 2007), adipocytes and stellate cells (Yin et al., 2013). As a result, the subgroups of CAFs are highly heterogenous which makes it difficult to identify a specific population of CAFs in TME (Fiori et al., 2019). Currently recognized biological hallmarks of CAFs include α-SMA, fibroblast-specific protein 1 (FSP1/S100A4), platelet-derived growth factor receptor (PDGFR) and type-I collagen etc. (Sugimoto et al., 2006).

Briefly, the intricate mechanisms of antineoplastic drug resistance mediated by CAFs can be summarized into the following aspects: (1) secreting soluble factors; (2) remodeling extracellular matrix (ECM); (3) reprogramming the metabolic process of tumor cells; (4) inducting epigenetic modifications of tumor cells; (5) delivering exosomes.

Secreting Soluble Factors

It has been proven that CAFs can secret various cytokines or factors which enable to activate a series of signaling cascades, leading to drug resistance and tumor cells relapse eventually. CAFs secrete diverse growth factors (including fibroblast growth factor, hepatocyte growth factor, transforming growth factor, and stromal cell derived factor), cytokines (such as IL-6, IL-8, IL-10 etc.), chemokines and protease (Figure 2; Mathot et al., 2017).

FIGURE 2
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Figure 2. Cancer-associated fibroblasts and drug resistance. The intricate mechanisms of drug resistance mediated by CAFs include secreting soluble factors, delivering exosomes, metabolic reprogramming and extracellular matrix (ECM) remodeling. CAFs can secret a broad range of cytokines or factors which enable to activate a series of signaling cascades, leading to therapeutic resistance. CAFs-derived exosomes deliver miRNAs, lncRNAs and mtDNA to cancer cells, which participate in transmitting paracrine signals of therapeutic resistance. Moreover, in order to adapt to a glucose-deficient microenvironment, CAFs coordinate with tumor cells to modulate metabolic mode. Lastly, activated signals within CAFs increased production of extracellular matrix components, resulting in changes of its physical and biochemical characteristics under therapeutic pressure. CCL1, chemokine C-C motif ligand-1; CCL5, chemokine C-C motif ligand-5; IL-6, interleukin-6; IL-8, interleukin-8;IL-11, interleukin-11; SDF1, stromal cell derived factor-1; HGF, hepatocyte growth factor; TGF-ß, transforming growth factor-β; IGF-2, insulin-like growth factor 2; PAI-1, plasminogen activator inhibitor-1, MMP, matrix metalloproteinase; HA, hyaluronan; HSPG2, heparin sulphate proteoglycan 2; LPP, lipoma-preferred partner. The figure was created with BioRender.com.

IL-6 was described to induce drug resistance. Multiple pathways such as nuclear factor-κB (NF-κB), JAK/STAT3, PI3K/AKT have been activated under therapeutic pressure in breast cancer and non-small cell lung cancer (Mao et al., 2015; Shien et al., 2017). Secretion of IL-6 causes the upregulation of C-X-C motif chemokine receptor 7 (CXCR7) through STAT3/NF-κB pathway. The expression of CXCR7 in esophageal squamous cell carcinoma tissues from chemotherapy resistant patients was significantly higher than that of chemotherapy sensitive patients (Qiao et al., 2018). In addition, the potential of IL-6 to drive epithelial-mesenchymal transition (EMT) has been identified in esophageal adenocarcinoma (Ebbing et al., 2019). IL-8 is another cytokine relating to CAFs. High levels of IL-8 were detected in gastric cancer patients who were insensitive to platinum-based therapy, which was associated with NF-κB activation and increased expression of ATP-binding cassette subfamily B member 1 (ABCB1) (Zhai et al., 2019). Moreover, in gastric cancer and lung adenocarcinoma, CAFs drive chemoresistance through IL-11 secretion via IL-11/STAT3/Bcl2 signaling pathway (Tao et al., 2016; Ma et al., 2019).

Stromal cell derived factor-1 (SDF-1) was found to be overexpressed in CAFs and played an essential role in tumor cell metastasis and chemoresistance by activating its receptor chemokine receptor 4 (CXCR4) (Orimo and Weinberg, 2006; Teng et al., 2016; Zou et al., 2017). The expression level of SDF-1 in CAFs was regulated by microRNA mir-1 negatively, with NF-κB and Bcl-xL signaling pathways involved in lung cancer chemoresistance (Li et al., 2016). Wei et al. found that SDF-1 secreted by CAFs promoted chemoresistance through paracrine induction of special AT-rich sequence-binding protein 1 (SATB-1) in pancreatic tumor cells. In turn, SDF-1/CXCR4/SATB-1 axis helped to maintain CAFs characteristics. Therefore, a reciprocal feedback loop was formed (Wei et al., 2018).

Transforming growth factor-β (TGF-β) expression in cancers is generally regarded as an important therapeutic target because it plays a key role in regulating the proliferation, differentiation and survival of cancer cells (Ciardiello et al., 2020; Li et al., 2020). CAFs conferred esophageal squamous cell carcinoma cells significant chemoresistance by activating FOXO 1, a member of the forkhead transcription factors in the O-box sub-family, inducing the secretion of TGF-β1 (Zhang H. et al., 2017). Hypoxia-inducible factor (HIF-1α) has been shown to synergize with CAFs paracrine signals, namely TGF-β2, to activate hedgehog transcription factor GLI2 in cancer stem cells (CSCs), leading to enhanced stemness/dedifferentiation and intrinsic resistance to chemotherapy of colorectal cancer (Tang et al., 2018). Apart from their assembly effect, CAFs also play a part in HIF-1 pathway modulation which mediates the photodynamic treatment resistance of colorectal cancer (Lamberti et al., 2019).

Hepatocyte growth factor (HGF) is one of the growth factors derived from CAFs. Recent evidence has revealed the role of HGF in transmitting resistance to epidermal growth factor receptor (EGFR) targeted therapy in lung cancer (Kasahara et al., 2010; Yi et al., 2018). HGF was identified to be a major mediator of CAFs induced resistance to EGFR tyrosine kinase inhibitor (EGFR-TKI) (Apicella et al., 2018; Suzuki et al., 2019). HGF derived from CAFs activated the c-Met/PI3K/Akt and glucose-regulated protein 78 (GRP78) pathways of SKOV3 and HO-8910 cells to attenuate the inhibition of cell proliferation and apoptosis caused by paclitaxel (PAC). Furthermore, HGF induced drug resistance has been validated in nude mice (Deying et al., 2017).

Cancer-associated fibroblasts have been found to constrict cisplatin-induced ovarian cancer cell apoptosis through activating STAT3 signaling (Yan et al., 2016). Consistently, another study demonstrated that cisplatin resistance in ovarian cells was attributed to the secretion of chemokine C-C motif ligand-5 (CCL5) by CAFs. Its molecular mechanism related to enhanced STAT3 and PI3K/Akt phosphorylation levels in ovarian cells (Zhou B. et al., 2016). Chemokine C-C motif ligand-1 (CCL1), combining exclusively with chemokine (C-C motif) receptor 8 (CCR8), is an inflammatory factor. However, its role has already gone beyond inflammation (Korbecki et al., 2020). Li et al. (2018) suggested that CCL1 participated in CAFs mediated chemoresistance by activation of TGF-β/NF-κB signaling pathway in colorectal cancer.

Besides the factors mentioned above, CAFs are capable of secreting many other humoral elements to induce therapeutic resistance. Evidence of increased expression of insulin-like growth factor 2 (IGF2) and insulin-like growth factor receptor-1 (IGF-1R) in CAF accumulating-lung cancer tissues proved that CAFs promote chemoresistance through IGF2/IGF-1R signal. It led to the activation of AKT/SoX2 pathway, elevating the expression of P-glycoprotein, decreasing drug retention and increasing drug efflux ultimately (Zhang Q. et al., 2018). Midkine (MK) is a kind of heparin-binding growth factor, promoting carcinogenesis and chemoresistance. CAFs in TME lead to high levels of MK in tumors. As a result, CAF-derived MK can induce cisplatin resistance through increased expression of lncRNA (Zhang D. et al., 2017). It has also shown that cisplatin treatment triggered the AKT and ERK1/2 signal cascades in esophageal squamous cell carcinoma cells mediated by releasing of plasminogen activator inhibitor-1 (PAI-1) from CAFs. The study confirmed that there is relevance between elevated PAI-1 level in CAFs and poor progression-free survival after therapy (Che et al., 2018). When cultured head and neck squamous cell carcinoma (HNSCC) cell lines with CAFs, cetuximab resistance was induced and elevated level of matrix metalloproteinase-1 (MMP-1) was detected, and the resistance can be reversed by using MMP inhibitor. The result suggested that drug resistance was achieved by CAFs derived MMP family (Johansson et al., 2012).

Remodeling Extracellular Matrix

Extracellular matrix is a dynamic system which changes its physical and biochemical characteristics under pathological conditions, for example, its molecular composition and elasticity (Gilbert et al., 2010). ECM can also sufficiently impede drug delivery by increasing microvascular endothelial cell remodeling (Figure 2). A study on ovarian cancer chemoresistance showed that CAFs increased the expression of lipoma-preferred partner (LPP) in endothelial cells through microfibrillar associated protein 5 (MFAP5)/FAK/ERK/LPP signaling pathway. Mechanically, LPP enhanced the formation of focal adhesion and stress fibers, promoting the mobility and permeability of endothelial cells. As a result, paclitaxel delivery to malignant cells has been decreased via increased intra-tumoral microvascular leakiness (Leung et al., 2018). In addition, hyaluronan (HA) has also been found to participate in remodeling extracellular matrix by producing high interstitial fluid pressure (IFP) to reduce the amount of drug exchange through capillaries (Paunescu et al., 2011; Jacobetz et al., 2013). CAFs are involved in producing HA in a TGF-β dependent manner (Sapudom et al., 2020). Meanwhile, CAFs are found to delay cancer cell response to chemotherapy through another critical component in matrix, heparin sulfate proteoglycan 2 (HSPG2). Stromal deposition of HSPG2 was partly mediated by NF-κB signaling, which enhanced the invasion, metastasis of pancreatic cells and induced gemcitabine resistance (Vennin et al., 2019). CAFs in BRAF mutant melanoma may participate in resistance to BRAF inhibitor PLX4720 by generating fibronectin-rich matrix. Melanoma-associated fibroblasts conferred PLX4720 tolerance dependent on the upregulation of integrin-β1 and the activation of focal adhesion kinase (FAK)/Src/ERK signaling pathway (Hirata et al., 2015).

Reprogramming the Metabolic Process of Tumor Cells

The abnormal proliferation of tumor cells relies on the enhanced adaptation to the nutritional microenvironment mediated through reprogrammed metabolic process. As a result, alterations in energy metabolism are considered to be one of the characteristics of tumor cells (Hanahan and Weinberg, 2011). In order to adapt to a glucose-deficient microenvironment, cancer cells undergo a metabolic switch to aerobic glycolysis, also known as the Warburg effect (Siska et al., 2020). Lactate is the end product of aerobic glycolysis and increased lactate production in MET/EGFR TKI-resistant breast cancer cells has been observed. Interestingly, lactate served as a critical media between breast cells and CAFs. Specifically, lactate uptake by CAFs activates NF-κB signals of CAFs, resulting in the upregulation of HGF. In turn, increased HGF turns on MET signals in cancers and confers resistance to TKIs (Apicella et al., 2018).

Although Warburg effect is a distinctive character of tumor cells, recent studies showed that other metabolic features, notably the reverse Warburg effect, metabolic symbiosis, and glutamine metabolism, pose challenges to antitumor therapy due to adaptive or acquired drug resistance (Figure 2; Yoshida, 2015). Migneco proposed a new model for understanding the reverse Warburg effect, in which glycolytic CAFs secreted pyruvate/lactate used by adjacent epithelial cancer cells as a source of mitochondrial tricarboxylic acid cycle (TCA) cycle, oxidative phosphorylation and ATP production. The result suggested that metabolic products produced by glycolytic CAFs promote tumor cells to escape from antiangiogenic drugs via decreasing the reliance of cancer cells on a vascular blood supply (Migneco et al., 2010). Metabolic symbiosis of CAFs with epithelial cancer cells has been identified in (monocarboxylate transporter 1) MCT1-positive prostate tumor cells and MCT4-positive CAFs (Pértega-Gomes et al., 2014). MCT4-positive hypoxic cells create a low PH acidic microenvironment through aerobic glycolysis and secreting lactate, while MCT1-positive oxidative cells take up lactate as a substrate for TCA cycle, which is termed as metabolic symbiosis (Montenegro and Indraccolo, 2020). Besides, it has been proved that angiogenesis inhibitors resistance mediated by metabolic symbiosis was dependent on mTOR signaling (Allen et al., 2016; Jiménez-Valerio et al., 2016). Tumor cells also achieve metabolic process via glutamine metabolic reprogramming. For example, in prostate cancer, the increase in glutamine synthesis after macropinocytosis of extracellular fluid was detected in CAFs, which was related to the cascade activation of RAS signaling. In turn, CAFs-secreting glutamine promoted mitochondrial metabolism in prostate cancer cells, inducing neuroendocrine differentiation, facilitating the development of resistance to androgen deprivation therapy (ADT). In consistence, prostate cancer patients with ADT resistance displayed increased blood glutamine level than those with satisfactory treatment outcomes (Mishra et al., 2018).

Inducting Epigenetic Modifications of Tumor Cells

Accumulating evidence underscores the epigenetic modification of tumor cells induced by CAFs plays a part in drug resistance. Dysregulated DNA methylation in CAFs has been reported to be concerned with breast cancer, stomach cancer and pancreatic cancer (Liu M. et al., 2017). It is proved that DNA methylation level in stromal cells is related to that of adjacent cancer cells (Hanson et al., 2006; Rodriguez-Canales et al., 2007). Soluble factors secreted by CAFs obviously upregulated the level of methylated CpGs on their regulated gene region (372 genes) in breast cancer cells, which shed light on the importance of epigenetic modifications of tumor cells induced by CAFs (Mathot et al., 2017). In addition, factors derived from CAFs were capable to induce reversible DNA hyper- and hypo-methylation during (epithelial-to-mesenchymal transition) EMT and (mesenchymal-to-epithelial transition) MET, leading to castration resistance and cancer stem cells expansion, predicting poor prognosis in prostate cancer (Pistore et al., 2017). Much evidence has already proven that EMT and stemness are also major contributors to drug resistance (Shibue and Weinberg, 2017; Nilsson et al., 2020). Moreover, EMT process was mediated by TGF-β derived from CAFs. Extensive methylation changes following TGF-β releasing were detected in ovarian cancer cells. Treatment with DNA methyltransferases inhibitor blockades DNA methylation in the EMT process (Cardenas et al., 2014). To develop a better therapeutic approach, a deeper knowledge of the impact of epigenetic regulation on the tumor microenvironment is necessary for combining epigenetic and checkpoint blockage therapies.

Delivering Exosomes

Cancer-associated fibroblasts derived exosomes have also emerged as active mediators of cancer progression and drug resistance by transmitting paracrine signals. Exosomes are membrane vesicles with a diameter of approximately 30-100 nm, containing protein, DNA, mRNA and miRNA (Fu et al., 2016; Kalluri, 2016; Li and Nabet, 2019). Exosomes are taken up by adjacent cells through endocytosis and act on the recipient cells. Recent studies have proven that exosomes are involved in the dynamic interplays between CAFs and cancer cells to promote tumor progression and chemoresistance (Figure 2; Ren et al., 2018).

Dysregulation of miRNAs in CAFs and the transfer of exosomal miRNAs between cancer cells and the microenvironment are associated with chemoresistance in multiple cancer types (Tanaka et al., 2015; Zhang L. et al., 2018; Qin et al., 2019; Guo et al., 2020). In pancreatic cancer, gemcitabine (GEM) treatment induced resistant CAFs that released exosomes containing SNAI1 and miRNA 164a. SNAI1 expression in exosomes was significant in inducing EMT. Moreover, the resistance can be reversed by treatment with GW4869, an inhibitor of exosome release (Richards et al., 2017; You et al., 2019). miRNA 106b was delivered directly from CAFs to pancreatic tumor cells via exosomes, leading to GEM insensitivity of tumor cells by targeting TP53INP1 (Fang et al., 2019). Except for miRNA 164a and miRNA 106b, miRNA 21 was also reported in GEM-induced chemoresistance of pancreatic cancer (Zhang L. et al., 2018). In ovarian neoplasm, miRNA 21 derived from CAFs and cancer associated adipocytes was transferred to cancer cells, which conferred paclitaxel resistance by directly targeting apoptotic protease activating factor-1(APAF1) (Yeung et al., 2016). Further, it has been demonstrated that cisplatin and paclitaxel treatment of gastric cancer promoted the secretion of miRNA 522 from CAFs, with the activation of ubiquitin-specific protease 7 (USP7)/heterogeneous nuclear ribonucleoprotein A1 (hnRNPA1) axis, resulting in arachidonate lipoxygenase 15 (ALOX15) inhibition and ultimately decreased chemo-sensitivity (Zhang H. et al., 2020). Additionally, miRNA 27a/b over-expressed CAFs in esophageal cancer microenvironment were correlated with cisplatin resistance by upregulation of TGF-β (Tanaka et al., 2015). In head and neck cancer, cisplatin resistance was found to be linked exosomal miRNA 196a and its targets, CDKN1B and ING5 (Qin et al., 2019).

Long non-coding RNA signatures of tumor-derived exosomes have been identified to be responsible for drug resistance. Exosome-enriched lncRNA H19 and colorectal-associated lncRNA can be transferred from CAFs to adjacent colorectal cells, inducing stemness of CSC and chemoresistance by activating Wnt/ß-catenin signaling pathway (Ren et al., 2018; Deng et al., 2020). Besides, mitochondrial DNA (mtDNA) transfer from CAFs to hormonal therapy-resistant breast cancer cells occurred via exosomes. Specifically, cancer cells with impaired metabolism received the exosomes loaded with full mitochondrial genome, causing restoration of oxidative phosphorylation. The delivery of mtDNA promoted resistance to hormone therapy and induced self-renewal potential of breast cancer cells (Sansone et al., 2017).

In short, exosomes transfer and secretion of soluble molecules constitute a major communication channel between CAFs and tumor cells as well as other stromal components in TME, which promotes cancer progression and therapeutic resistance.

Based on these multiple effects of CAFs on drug resistance (Table 1), CAF have become an interesting therapeutic target for cancer intervention. Here, we will briefly discuss the main advances in CAF-targeted therapeutic strategies. Firstly, direct elimination of CAFs can significantly enhance the efficacy of chemotherapy. Co-delivery of cyclopamine (CPA), a kind of sonic hedgehog inhibitor, and paclitaxel (PTX) by construction of polymeric micelle (M-CPA/PTX) shows promising therapeutic outcomes for Pancreatic ductal adenocarcinoma (PDAC). M-CPA can deplete CAFs and modulate stroma thus to enhance the cytotoxic activity of PTX. In vivo, the compounds remarkably prolonged the survival time and inhibited tumor growth (Zhao et al., 2018). However, in a hybrid mouse model of spontaneous PDAC mice with α-SMA thymidine kinase (TK) transgenic mice, depletion of myofibroblasts reduced the production of type I collagen and altered ECM, with enhanced tumor hypoxia, immunosuppression and reduced survival (Özdemir et al., 2015). From this point of view, it seems that we need to be more cautious about the strategy of exhausting CAFs. Secondly, given the potential risks of depleting CAFs, normalization or inactivation of activated CAFs is another choice for regulating the functions of CAFs. By loading fibroblast activation protein-α (FAP-α) antibody and CXCL12 siRNA onto the peptide nanoparticles (PNP), the nanosystem (PNP/siCXCL12/mAb) can selectively downregulate the expression of CXCL12 in CAFs via FAP-α recognition, causing inactivation of CAFs and blockade of CAFs-related tumor metastasis. As such, attempts to inactivate or normalize CAFs rather than diminish them, may be more preferable approaches and can promote the development of novel anticancer therapy. Thirdly, it is feasible to restore chemotherapy sensitivity of tumor cells by blockading the cross-talk between CAFs and tumor cells. IL-1β and TGF-β1 pathways are involved in CAFs recruitment and polarization. Simultaneous inhibition of IL-1β and TGF-β1 pathways with TAK1 inhibitor plus TGFBR1 inhibitor could restrain the activation of NF-κB, reduce the secretion of IL-6 and IL-11, and sensitize colorectal cancer tumor cell line (DLD1) to oxaliplatin. In vivo, the combined therapy diminished colorectal tumor cells metastasis and CAFs aggregation (Guillén Díaz-Maroto et al., 2019).

TABLE 1
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Table 1. Mechanisms of antitumor drug resistance mediated by CAFs.

Immune Inflammatory Cells and Drug Resistance

Tumor Associated Macrophages (TAMs)

Tumor associated macrophages are the most abundant immune cells found in TME (Perrotta et al., 2018; Najafi et al., 2019). Increased TAMs infiltration within TME is declared to be concerned with poor prognosis and unsatisfactory response to chemotherapies for cancer patients (Sugimura et al., 2015; Li et al., 2019). TAMs derive from the circulating Ly6C+CCR2+ monocytes. TAMs are characterized with great heterogeneity in TME and they can be separated into two subgroups conventionally: M1 and M2 (Liu and Cao, 2015). M1-type macrophages are activated via classical pathway while M2-type macrophages are alternatively activated. In general, the role of M2 phenotype is defined to promote tumor progression and drug resistance, to produce anti-inflammatory cytokines, and to induce Th2 response. Macrophage polarization from M1 to M2 state is common in cancer condition educated by microenvironment (Moradi-Chaleshtori et al., 2020).

The interaction between tumor cells and TAMs which associated with therapeutic resistance lies on that tumor cells promote TAMs to differentiate into immunosuppressive M2-polarized macrophages under treatment pressure. In turn, M2 TAMs endow cancer cells with acquired chemoresistance through diverse mechanisms. IL-34 secreted by chemo-resistant tumor cells in a paracrine manner enhanced the polarization of M2 TAMs by activating colony stimulating factor 1 receptor (CSF1R)/AKT signaling pathway (Baghdadi et al., 2016). Besides, elevated expression of macrophage inhibitory factor (MIF) was detected in cisplatin resistant lung cancer cells, which mediated M2 polarization of TAMs through Src/CD155/MIF signaling (Huang et al., 2019). In aromatase inhibitors resistant breast cancer cells, Jagged1-Notch pathway was activated, leading to macrophage differentiation toward M2 TAMs and upregulated expression of IL-10. M2 TAMs, in turn, contributed to the acquisition of drug resistance and metastasis (Liu H. et al., 2017). In gastric cancer treated with 5-fluorouracil (5-FU), transformation of M2-type TAMs was ascribed to accumulation of reactive oxygen species (ROS), activating hypoxia-inducible factor 1α (HIF-1α) signaling, driving the expression of high-mobility group box 1(HMGB1). As a result, tumor-protected M2-type TAMs produced growth differentiation factor 15 (GDF15) to enhance the fatty acid β-oxidation in tumor cells, which induced chemoresistance (Yu et al., 2020).

Like CAFs, TAMs secret numerous soluble factors into TME to protect tumor cells from drug attack, including enzymes, exosomes, interleukins, chemokines etc. It was found that cathepsin B and S expressing macrophages protected against paclitaxel-induced tumor cells death. The combined application of paclitaxel and cathepsin inhibitor can effectively enhance the therapeutic effect (Shree et al., 2011). Halbrook et al. (2019) pointed that alternatively activated TAMs secreting a series of pyrimidine nucleosides conferred pancreatic tumor cells resistance to gemcitabine, through molecular competition at the level of drug uptake and metabolism. TAMs also induced upregulation of cytidine deaminase, mediating inactivation of gemcitabine (Weizman et al., 2014). In colorectal cancer cells, 5-fluorouracil (5-FU) promotes the production of putrescine by TAMs. As a result, putrescine endows resistance to 5-FU by inhibiting the activation of p-JNK/caspase-3 apoptosis pathway (Zhang et al., 2016). M2-polarized TAMs are found to produce NO to protect tumor cells from apoptosis induced by cisplatin. The mechanism lies on NO/cGMP/PKG signaling pathway, leading to the inhibition of acid sphingomyelinase (Perrotta et al., 2018). Exosomal transfer of miRNA from macrophages to tumor cells has been noted as well. TAMs-derived exosomes transfer miR-365 to pancreatic adenocarcinoma cells to elicit gemcitabine resistance, which is performed by enhanced expression of triphosphate nucleotide and cytidine deaminase (Binenbaum et al., 2018). In addition, exosomes containing miR-223 and miR-21 are demonstrated to be associated with PTEN-PI3K/AKT signaling pathway in cisplatin chemoresistance of epithelial ovarian cancer and gastric cancer cell, respectively (Zheng et al., 2017; Zhu et al., 2019). Macrophages are usually recruited into TME and secret various chronic inflammatory cytokines, both pro-inflammatory and anti-inflammatory factors. Angst et al. (2008) highlighted that TAMs protect pancreatic cancer cells from apoptosis by secreting IL-1ß, a pro-inflammatory cytokine, increasing the expression of cyclooxygenase-2 (COX-2) and prostaglandin E2 (PGE2) through activating MAPK and ERK1/2 pathway. It has been observed that the dysregulation of miR155-5p/C/EBPb/IL-6 signaling in TAMs was responsible for chemoresistance in colorectal cancer. As a result, TAMs secreted IL-6 to activate IL-6R/STAT3/miR-204-5p signaling pathway in tumor cells (Yin et al., 2017). Hedgehog pathway inhibitor cyclopamine treatment increased the infiltration of M2-type TAMs in breast cancer, attenuating the efficacy of chemotherapy due to the accumulation of IL-6 (Xu X. et al., 2019). Besides, IL-10/STAT3/bcl-2 signaling pathway has been proven to be linked with breast cancer cell resistance to paclitaxel. Inhibition of TAMs derived-IL-10 using neutralizing antibody significantly enhanced sensitivity of breast cancer cells (Yang et al., 2015). The cross-talk between TAMs and HNSCC cells was mediated by IL-6 and C-C motif chemokine ligand 15 (CCL15). HNSCC cells secret (vascular endothelial growth factors) VEGF to recruit macrophages and induce their polarization by secreting IL-6. Polarized TAMs produce CCL15 to weaken the sensitivity of tumor cells to gefitinib via CCL15/CCR1/NF-κB signaling pathway (Yin et al., 2019).

Targeting of immune-regulatory receptors, for example, programmed cell death protein-1 (PD-1) and its ligand PD-L1, as well as cytotoxic T-lymphocyte-associated antigen-4 (CTLA-4), reduces T cell suppression, and relives T cell function, thereby restoring antitumor immunity. However, accumulating reports have displayed that TAMs may account for drug resistance to immune checkpoint blockades (ICBs). Wu et al. demonstrated HIF-1α enhanced the level of triggering receptor expressed on myeloid cells-1 (TREM-1) of TAMs. On the one hand, TREM-1+ TAMs damaged the cytotoxic functions of CD8+ T cells and caused CD8+ T cell apoptosis, in a PD-1/PD-L1 dependent manner. On the other hand, TREM-1+ TAMs recruited abundant CCR6+Foxp3+ Tregs into TME via CCL20/ERK/NF-κB pathway. Application of TREM-1 signaling inhibitor GF9 statistically decreased CCR6+Foxp3+ Tregs infiltration, increasing the therapeutic efficacy of ICBs, as a result postponed tumor progression (Wu et al., 2019). Aside from negatively regulating CD8+ T cells, TAMs also interfere the function of CD4+ T cells. It was reported that the mechanisms of glioma cells resistance to anti-PD-1 and anti-CTLA-4 were mediated by TAMs through PD-1/PD-L1/CD80 axis, accompanied by Treg accumulation. Co-culture of naïve CD4+ T cells with PD-L1-positive TAMs induced the expression of CD80 on CD4+T cells. PD-L1/CD80 interaction blockades antitumor immune responses to anti-PD-1 and anti-CTLA-4 therapies (Aslan et al., 2020).

Evidence from prostate cancer treated by ADT demonstrates that the interconnection between TAMs and CSCs can also lead to drug resistance. CSCs are capable of remodeling macrophages toward TAMs. Reciprocally, TAMs enhanced the stem-like characteristics of CSCs and drug resistance via IL-6/STAT3 signaling pathway (Huang et al., 2018). Consistent with this finding, in C57BL/6 mice model inoculated with MC38-CSCs (colon tumor) and 3LL-CSCs (lung cancer), TAMs generated milk-fat globule epidermal growth factor-VIII (MFG-E8) to regulate CSCs. MFG-E8 cooperated with IL-6 to stimulate STAT3 and hedgehog signaling pathways in CSCs, driving anticancer drug resistance (Jinushi et al., 2011). Moreover, the EMT induced by TAMs could be a potential mechanism amplifying peritoneal dissemination and causing chemoresistance in pancreatic cancer (Kuwada et al., 2018).

In conclusion, the mechanisms involved in antitumor drug resistance mediated by TAMs include release of multiple cytokines, transformation toward suppressive-M2 phenotype, suppressive effects on immune cells, modulation of CSC properties and promotion of EMT, which have been summarized in Table 2.

TABLE 2
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Table 2. Mechanisms of antitumor drug resistance mediated by TAMs.

Furthermore, tumor-associated neutrophils (TANs) high infiltration within TME was related to tumor progression and drug resistance (Incio et al., 2016). Neutrophil polarization may affect their role in the tumor microenvironment. Similar to the classification of M1/M2 macrophages, TANs are sorted into antitumorigenic N1 phenotype and pro-tumorigenic N2 phenotype on the basis of their functional differences (Zhang Y. et al., 2020). TGF-β and type I IFN-γ were suggested to play essential roles in the polarization of TANs switching from N1 to N2 (Fridlender et al., 2009; Pylaeva et al., 2016). CXCL5 serves as a key factor in recruiting TANs (Nywening et al., 2018). Sorafenib administration led to increased secretion of CXCL5 derived from HCC cells, inhibiting TANs apoptosis by inducing HIF1 α/NF-κB/CXCL5 pathways, enhancing TAN infiltration in both animal models and HCC patients. Besides, HCC cells were able to polarize TANs and promote secretion of CCL2 and CCL17 by TANs through activating PI3K/Akt and p38/MAPK signals. As a response to HCC cells, TANs facilitate intra-tumoral infiltration of CCR2+macrophages and CCR4+Treg cells via CCL2-CCR2 and CCL17-CCR4 connections (Zhou S.L. et al., 2016). Therefore, combined blockade of TANs and TAMs present advantages in improving therapeutic outcomes (Nywening et al., 2018).

Generally, there are three approaches to target TAMs: reduced recruitment, direct depletion, and repolarization. CCL2 is a potent chemokine for monocytes recruitment and CCL2-CCR2 axis is the primary mediator for the expansion of macrophages in TME. In a PDAC mouse model, tumor cells-derived CCL2 inhibited the efficacy of ablative radiotherapy by recruiting inflammatory monocytes/macrophages into the TME to accelerate tumor proliferation and angiogenesis. While selective blockade of CCL2 using neutralizing antibodies interrupted the recruitment of monocytes/macrophages and produced synergistic antitumor effects with radiotherapy and prolonged survival time (Kalbasi et al., 2017).Next, colony-stimulating factor 1 receptor (CSF1R), receptor of CSF-1 and IL-34, is necessary for the proliferation, differentiation and survival of macrophages (Muñoz-Garcia et al., 2021). Therefore, avenues of targeting CSF-1R alone or combined with standard therapies seem to be feasible. Enhanced infiltration of TAMs was observed after radiotherapy in gliomas mouse model, which was responsible for tumor recurrence. While combined therapies of CSF-1R inhibitor, BLZ945, with radiotherapy significantly delayed glioma relapse. Particularly, CSF-1R could inhibit both resident-microglia and recruited monocyte-derived macrophage. Neutralizing antibody of CD49d could only inhibit the recruitment of monocyte-derived macrophage without effect on resident microglia. Compared to the CD49d neutralizing antibody, CSF-1R displays stronger efficacy in delaying relapse (Akkari et al., 2020). Nevertheless, existence of antigen presenting cells (APCs) including macrophages and dendritic cells (DCs) are essential for T cells activation. Elimination of macrophages could reduce the efficacy of immunotherapy (Diggs et al., 2020). Repolarization of TAMs by phenotype switch from M2 to M1 provides an opportunity to balance immune microenvironment, and compensates for the disadvantages of depletion of all macrophages. In 4T1 breast cancer mouse model, selectively targeting M2 TAMs, by simultaneously delivery of CSF-1R and CD47/SIRPα inhibitors via dual-inhibitor-loaded nanotherapeutic technique, results in increased M2 repolarizations into M1, enhanced phagocytosis activity, and satisfactory anticancer outcome (Ramesh et al., 2019). This preclinical trial suggests a promising and preferable strategy of targeting TAM.

Myeloid-Derived Suppressor Cells (MDSCs)

Myeloid-derived suppressor cells are an immature heterogeneous population of the myeloid family, which contain two subsets of cells. One group is defined as granulocytic-MDSCs (G-MDSCs), with the CD11b+Ly-6G+Ly-6Clow phenotype, expressing high levels of arginase-1 (Arg-1). This population are also termed as PMN-MDSC due to their polymorphonuclear (PMN) morphology. The other group is identified as monocytic-MDSCs (Mo-MDSCs) because of their monocytic-like morphology, with the CD11b+Ly-6GlowLy-6Chi marker (Youn et al., 2008; Talmadge and Gabrilovich, 2013).

One of the main features of MDSCs is immunosuppression (Figure 3). MDSCs lead to the inhibition of different types of immune cells, but the primary targets of MDSCs are T cells. The factors participated in MDSCs-mediated immunosuppression including Arg-1, IL-23, IL-10, TGF-β, PGE2, and many others (Gabrilovich, 2017; Xu et al., 2017). Recent studies elucidated that the reciprocal action between malignant cells and MDSCs plays a critical role in immunosuppressive chemoresistance. The level of PMN-MDSC and Arg-1 in serum of multiple melanoma (MM) patients was higher than that of healthy individuals. Furthermore, PMN-MDSC extracted from MM patients could suppress the activation of T cells effectively and protect MM cells from bortezomib treatment. However, this protection was offset by Arg-1 inhibitor (Romano et al., 2018). Mechanically, MM cells survival induced by MDSCs is dependent on AMPK activation, MCL-1 and BCL-2 expression in myeloma cells (De Veirman et al., 2019). In addition, it has been elucidated that the acquired ADT resistance of prostate cancer could be blamed on IL-23 secreted by MDSCs. IL-23-IL-23R-RORγ axis activated the androgen receptor pathway in prostate cancer cells, regulating resistance to ADT (Calcinotto et al., 2018).

FIGURE 3
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Figure 3. Interactions of tumor cells with parts of non-malignant cells within tumor microenvironments mediating drug resistance. Tumor microenvironment contains quantities of non-malignant stromal cells which are essential for tumor progression and drug resistance. Interactions between tumor cells and stromal cells polarize stromal cells. In turn, the stromal cells educated by tumor cells secret a variety of molecules, leading to immunosuppression, metabolic regulation and pharmacokinetics adjustment, which eventually weakens therapeutic efficacy. Arg-1, arginase-1; IL-23,interlukin-23; PNT, peroxynitrite; G-CSF, granulocyte-colony stimulating factor; PGE2, prostaglandin E2; FOXP3, forkhead box protein P3; mGlutR1, glutamate receptor 1; P-gP: P-glycoprotein, IDO1, indoleamine 2,3-dioxygenase; CAA: cancer associated adipocyte; FFAs: free fatty acids; AA: arachidonic acid; VEGF: vascular endothelial growth factor; FGF4: fibroblast growth factor 4; FAK: focal adhesion kinase. CTL, cytotoxic T lymphocytes. The figure was created with BioRender.com.

Besides the mechanisms mentioned above, tumor cells are found to recruit and activate MDSCs in TME under therapeutic pressure. In vitro and in vivo results as well as clinical samples demonstrated that the expression of granulocyte-colony stimulating factor (G-CSF) in cervical cancer cells was significantly linked with MDSC infiltration and chemoresistance (Kawano et al., 2015). Blockade of colony stimulating factor-1 receptor (CSF-1R) can prevent immune resistance to immunotherapy (Holmgaard et al., 2016). Doxorubicin resistant breast cancer cells escape immune surveillance by secreting PGE2. PGE2 then bind with its receptor on MDSCs, EP2/EP4, leading to accumulation of MDSCs. PGE2/miR-10/AMPK signaling pathway of MDSCs was activated, with inhibition of CD4+CD25 T cells and decreased production of IFN-γ (Rong et al., 2016). BRAF inhibitor-resistant melanomas induced expansion of CCR2-expressing monocytic-MDSCs in the TME by producing CCL2, activating MDSCs through MAPK signaling. Combination of checkpoint blockade with MDSC depletion significantly reversed BRAF inhibitor resistance (Steinberg et al., 2017). Of note, MDSCs not only play a part in functionally suppression of T cells, but also participate in (cytotoxic T lymphocytes) CTL-mediated cytolysis. Lu et al. (2011) demonstrated that MDSCs are a predominant origin of the free radical peroxynitrite (PNT) in lung, pancreatic, and breast cancer samples. PNT induces post-translational modifications of cell surface molecules while not affecting cell viability, inhibiting processed peptides presentation to tumor-associated MHC molecules. Thus, tumor cells escape from antigen-specific CTLs and acquire immunological resistance (Lu et al., 2011).

These findings suggest the important role of MDSCs (Table 3), which motivate us to consider them as a target to overcome tumor resistance. MDSCs can be diminished by using chemotherapeutic drugs. CD33 is identified as a pathological marker for recognizing MDSCs across cancer subtypes and is responsible for immunosuppressive microenvironment. Conjugating anti-CD33 antibody with toxin calicheamicin, so called as gemtuzumab ozogamicin, can deplete CD33+ MDSCs thus to restore T cell activity and reactive CAR-T cell response (Fultang et al., 2019). Meanwhile, this strategy shows good results in clinical trials (Lancet et al., 2020; Schlenk et al., 2020). Another approach to inhibit MDSCs is to block their signaling cascades. IL-1β is an upstream mediator of myeloid resistance. Anti-IL-1β significantly decrease the infiltration of PMN-MDSCs and TAMs in TME. The combined use of anti-IL-1β and anti-PD-1 or cabozantinib increased anti-tumor activity (Aggen et al., 2021). One of the most promising techniques for targeting MDSCs is to promote their reprogramming. Increased activation of PKR-like endoplasmic reticulum kinase (PERK) in MDSC contribute to MDSC-mediated T cell dysfunction by stimulating transcriptional factor NRF2. Inhibition of PERK interrupts cytosolic mitochondrial DNA-STING-type I IFN axis and converts MDSCs into normal myeloid cells with activated CTL immunity. PERK inhibitor combined with anti-PD-L1 therapy shows synergetic effects in B16 bearing mice (Mohamed et al., 2020).

TABLE 3
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Table 3. Mechanisms of antitumor drug resistance mediated by MDSCs.

T-Regulatory Lymphocytes (T-Reg)

Tregs are a subpopulation of immunosuppressive T cells identified as CD4+CD25+, and are characterized by expression of the Foxp3, which is essential for Tregs development and differentiation. In the TME, increased infiltration of Tregs has been defined to positively associate with poor prognosis and chemoresistance in melanoma, glioblastoma, HNSCC, ovarian, colorectal, renal and lung cancer (Bamias et al., 2008; Li et al., 2012; Schuler et al., 2013; Liu X.D. et al., 2015; Wang D. et al., 2019; Imbert et al., 2020; Long et al., 2020). Acquired resistance to ICBs remains a challenge in cancer therapy as a compensatory pathway emerges in TME to evade the antitumor effects induced by ICBs. Apart from the induction of MDSCs we summarized above, increased ratio of Tregs within TME suggests another cellular mechanism (Figure 3).

In vivo, 5-FU treatment elevated the expression of CCL20 in colorectal cancer cells (CRC) by activating FOXO1/CEBPB/NF-κB signaling, which promoted the recruitment of Tregs within TME. The proportion of CD4+Foxp3+ Tregs in tumor infiltrating lymphocytes (TIL) of CRC was dramatically higher than that of paired controls. Expression of Foxp3+ was obviously associated with resistance-related genes, including BCL2, WNT1, ATP8A2 and VIM. CCL20 blockers inhibit tumor progression and restore sensitivity to 5-FU of CRC (Wang D. et al., 2019). In vitro, mouse Lewis lung cancer (LLC) cells, overexpression of Foxp3+ was also identified to increase the IC50 values of Adriamycin (ADM) and mitomycin C (MMC) (Li et al., 2012). Moreover, recent evidences have proven that amino acid metabolism could affect immune cell response to tumor cells by regulating Tregs. Folgiero et al. (2016) disclosed that mTOR inhibitor, rapamycin, induces indoleamine 2,3-dioxygenase (IDO1) expression in medulloblastoma cells. IDO1, one of three enzymes catalyzing the degradation of TRP along the kynurenine pathway, led to Treg expansion by inducing CCL2 expression, creating an immune-tolerance microenvironment. VEGF inhibition is a critical method for inhibiting angiogenesis. While results showed that resistance to VEGF inhibitors is elicited by upregulation of Tregs. Specifically, the increased expression of glutamate/cystine antiporter SLC7A11/xCT causes elevated extracellular glutamate in the VEGF inhibitors treated glioblastoma cells, promoting Tregs proliferation, activation and suppressive function (Long et al., 2020). Indeed, high levels of ATP metabolism within TME have been determined to be linked with Tregs as well as immunosuppression (Deaglio et al., 2007). Experiments conducted by Gourdin et al. (2018) showed that CD73+CD4+ effector T cells (Teffs) act synergistically with CD39+Tregs to metabolize ATP to immunosuppressive adenosine, restraining the function of Teffs on IL-17A production. What is more, the compensatory mechanisms between CSF1R+ TAMs and Foxp3+ Treg cells promote resistance to tumor immunotherapeutic agents. Either reduction of CSF1R+ TAMs or Foxp3+ Tregs will limit the function of CD8+ T cells on tumor growth. Only co-blockade of CSF1R+ TAMs and Foxp3+ Tregs can obtain a synergistic effect on augmentation of CD8+ T cells and tumor suppression (Gyori et al., 2018).

Collectively, over time and as a result of stress selection, some tumors augment Tregs function by producing more self-antigens and acquire compensatory pathways to evade the antitumor therapy, as well as resistance to ICBs (Table 4). Therefore, a deeper comprehension of the mechanisms and molecular pathways by which ICBs regulate T cells and Tregs, is necessary to design better immunotherapeutic strategies. Therapeutic approaches depleting Tregs mainly focused on their molecular markers, such as CD25, CCR8. Treg depletion using anti-25 antibody combined with dual immunotherapy and radiotherapy restored antitumor immunity durably and induced immunologic memory (Oweida et al., 2018). Fc-optimized anti-human CCR8 antibody results in restrict Treg exhaustion without influence on Teffs (Campbell et al., 2021). CCR8-directed Treg elimination shows synergistic effect with PD-1 blockade in mouse model (Van Damme et al., 2021). In addition, CCR4 is a robust chemokine receptor for Treg recruitment in TME. Anti-CCR4 mAb (mogamulizmab) is under clinical investigation either as a monotherapy or combinational choice of anti-PD-1 mAb (Kurose et al., 2015; Doi et al., 2019).

TABLE 4
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Table 4. Mechanisms of antitumor drug resistance mediated by Tregs.

In summary, due to the presence of TAMs, MDSCs, Tregs and their related factors, immunosuppressive microenvironments are now considered a major obstacle to ICBs. A range of investigations on turning non-immunogenic tumors into immunogenic tumors have been developed, for example, combinations of ICBs with anti-angiogenic agents (Makker et al., 2019), targeted therapies (De Henau et al., 2016), and other checkpoint inhibitors (Bedke et al., 2021). These therapeutic strategies should maximize the effectiveness of immunotherapy and induce sustained anti-tumor immune responses, to reach better clinical outcomes and response rates in cancer patients.

Mesenchymal Stem Cells (MSCs)

Mesenchymal stem cells (MSCs), commonly called mesenchymal stromal cells, are one of another pivotal components of the TME (Shi et al., 2017). MSCs have been reported to be involved in many distinct steps of tumorigenesis, such as angiogenesis, metastasis, epithelial-mesenchymal transition, anti-apoptosis, pro-survival, immunosuppression and therapy resistance. A growing body of researches suggest the important role of MSCs in drug resistance. MSCs inherently possess the ability to be chemoresistance and can confer this resistance to many types of cancer cells, including osteosarcoma, acute lymphoblastic leukemia, breast cancer, ovarian cancer, oral squamous cell carcinoma, hepatocellular carcinoma and so on (Roodhart et al., 2011; Han et al., 2014; Ji et al., 2015; Xu et al., 2018; Lu et al., 2020; Raghavan et al., 2020; Wang S. et al., 2020). Apart from bone marrow, where MSCs were originally discovered, adipose tissue, peripheral blood, umbilical cord are also important sources of MSCs. As a heterogeneous group of progenitor cells, MSCs are known for the capacity to transdifferentiate into multicellular lineages including chondrocytes, osteocytes, adipocytes, myocytes, astrocytes, fibroblasts, and pericytes (Shan, 2004). Featured for their ability to adhere to the plastic, MSCs are also typically positive for certain patterns of surface markers (CD73, CD105, CD44, CD29, and CD90), concomitantly they lack expression of endothelial markers (CD34, CD31, and vWF) and hematopoietic markers (CD34, CD45, and CD14) (Reagan and Kaplan, 2011).

According to recent studies, MSCs can promote drug resistance in different ways as follows (Figure 4): (1) secreting soluble factors; (2) delivering MSC-exosomes; (3) genetic mutations in MSCs; (4) direct cell-cell contact; (5) differentiating into CAF or CSC.

FIGURE 4
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Figure 4. Mesenchymal stem cells and drug resistance. Mainly isolated from bone marrow, adipose tissue and umbilical cord, MSCs promote drug resistance in multiple ways, such as secreting soluble factors and exosomes, genetic mutations, direct cell-cell contact and differentiating into CAF or CSC. The diverse soluble factors and exosomes derived from MSCs could induce chemoresistance dependent on multiple pathways and downstream mechanisms, some of which relate to the inhibition of tumor cell apoptosis by regulating the expression of apoptosis-related proteins. It is noteworthy that chemoresistance properties of MSCs can be conferred via direct cell–cell contact with tumor cells as well. This interaction can enhance the expression of Bcl-2. Also, gene mutations such as p53 deficiency in MSCs could contribute to drug resistance by mediating antitumor immunity. Finally, MSCs have the potential to evolve into CAFs and CSCs, which have been reported to be involved in the development of resistance. MSC, mesenchymal stem cell; CSC, cancer stem cell; CAF, cancer-associated fibroblast; SDF-1: stromal cell-derived factor-1; TGF-β, transforming growth factor-β; PIFAs, platinum-induced fatty acids. ICAM-1, intercellular adhesion molecule-1. The figure was created with BioRender.com.

Secreting Soluble Factors

Mesenchymal stem cells can release diverse growth factors, cytokines and fatty acids which are involved in multiple pathways and downstream mechanisms, leading to the acquisition of drug resistance (Scherzed et al., 2011; Luo et al., 2014; Senthebane et al., 2017). As discussed earlier, increased IL-6 secretion by CAFs was described to induce chemoresistance. Similarly, MSCs derived IL-6 plays an important role in the resistance via the activation of downstream STAT3 cascades in different tumors. For example, in breast cancer, MSCs secreting IL-6 causes protection of MCF-7 cells from cisplatin-induced apoptosis, which is mediated by activating STAT3 signaling pathway with the markedly decreasing expression of Bax (Xu et al., 2018). In osteosarcoma cells, IL-6 produced by MSCs activates the JAK2/STAT3 signaling, with the subsequent up-regulation of multidrug resistance protein (MRP) and P-gP expression, which is relevant to poor response rates of clinical osteosarcoma chemotherapy (Tu et al., 2016). And in NPC, MSC-derived IL-6 was found to significantly upregulate STAT3 signal pathway, which could bind to the promoter region of NET5 gene, thus contributing to the increased expression of CD73. Subsequently, the elevated expression of CD73 promotes NPC tumor growth and inhibition of cisplatin-induced apoptosis, mediating resistance of NPC cells to cisplatin (Zeng et al., 2020). In head and neck carcinoma, other paracrine cytokines secreted by MSCs, including IL-6, IL-7, IL-8, and growth factors such as VEGF, have also been reported to be involved in the development of tumor drug resistance (Scherzed et al., 2011). IL-7 was demonstrated to be highly expressed by MSCs in chronic myeloid leukemia (CML). It is known that imatinib (IM) and nilotinib (NI) are remarkably effective therapeutic agent of BCR/ABL-positive CML and have improved the clinical outcomes. The IL-7-mediated JAK1/STAT5 pathway bypasses BCR/ABL signals, protecting tumor cells from imatinib (IM) and nilotinib (NI) in a BCR/ABL-independent way. Interestingly this could explain the early resistance before the BCR/ABL genetic mutation (Zhang et al., 2019). IL-8, a neutrophil chemoattractant, is one of the CXC chemokine receptors 1 and 2 (CXCR1/2) ligands. It has been reported that through highly releasing chemokine (C-X-C motif) ligand 1 (CXCL1), CXCL2, and IL-8, MSCs manipulate metabolic programs to promote M2 macrophages differentiation, leading to abolition of their tumoricidal functions, thus facilitating the acquisition of chemoresistance in ovarian tumor cells. As expected, CXCR1/2 inhibitor reparixin could revert MSC-mediated drug resistance in ovarian cancer by restoring the anti-tumoral function of macrophages both in vitro and in vivo. Hence, reparixin has the potential to improve the efficacy of carboplatin in cancer cells (Le Naour et al., 2020).

Another chemokine CXCL12, also named SDF-1, is constitutively secreted by MSCs. SDF-1a/CXCR4 interactions between CML cells and MSCs protect CML cells from imatinib-induced cell death by reducing activation of caspase-3 and promoting the expression of Bcl-XL, an important anti-apoptotic protein inhibited by imatinib (Vianello et al., 2010). SDF-1a/CXCR4 axis was also reported to mediated drug resistance in acute lymphoblastic leukemia (ALL). MSCs increase the secretion of CXCL12, accompanied with the elevated expression of surface CXCR4 on chemo-resistant leukemic cells in the presence of vincristine. Furthermore, vincristine induced ALL apoptosis can be attenuated by upregulating Bcl-2 and downregulating Bax. Interestingly, all of these could be effectively reversed by the CXCR4 antagonist, AMD3100, which blocks the SDF-1a/CXCR4 axis and then restores sensitivity of ALL to chemotherapy (Wang S. et al., 2020). In addition, MSCs derived SDF-1a was also noted to mediate the cross-talk with the ovarian cancer cells, thus inducing their thermotolerance from hyperthermia intraperitoneal chemotherapy, a selective therapeutic approach for ovarian carcinoma (Lis et al., 2011).

Fatty acids are another important factor released by MSCs. Researches have demonstrated that the MSCs induced chemoresistance could be mediated by secreting two unique platinum-induced fatty acids (PIFAs). These two distinct PIFAs, namely 12-oxo-5,8,10-heptadecatrienoic acid (KHT) and hexadeca-4,7,10,13-tetraenoic acid [16:4(n-3)] are reported to confer resistance to a broad spectrum of anticancer drugs in minor quantities. Interestingly, inhibition of the central enzymes (cyclooxygenase-1 and thromboxane synthase), associated with the production of PIFAs, significantly enhances the chemotherapy efficacy (Roodhart et al., 2011). While the exact mechanism by which MSCs derived PIFAs induce chemoresistance remains to be elucidated.

Apart from cytokines, chemokines and fatty acids, the expression of growth factors like TGF-β was also reported to be upregulated in MSCs. In hepatocellular carcinoma (HCC), the tumor inflammatory microenvironment stimulates the overexpression of TGF-β in MSCs, inducing chemoresistance of HCC cells by promoting autophagy. Knockdown the expression of TGF-β by transfecting siRNA attenuates the ability of MSCs to induced autophagy and restore the sensitivity to chemotherapy in HCC cell (Han et al., 2014). In gastric cancer (GC), evidence presents that MSCs secreted TGF-β1 promotes fatty acid oxidation (FAO) to support stemness features and drug resistance, which is mediated by activating SMAD2 and SMAD3 and promoting lncRNA MACC1AS1 expression (He et al., 2019).

Delivering MSC-Exosomes

Exosomes transferring a variety of bioactive molecules including mRNAs, miRNAs and proteins, play important roles in inter- and intra-cellular interplay through pathways that influence TME regulation and drug resistance (Zhang X. et al., 2017; Adamo et al., 2019). Accumulating evidence suggests that MSC-derived exosomes contribute to chemoresistance through different ways, including drug sequestration, delivering specific mRNA molecules and proteins, mediating communication between MSCs and cancer cells (Adamo et al., 2019).

Mesenchymal stem cell-derived exosomes are reported as important mediators of drug resistance in gastric cancer. MSC-exosomes incorporate into the gastric cancer cells, stimulating the activation of CaM-Ks (predominantly CaM-KII and CaM-KIV), triggering downstream Raf/MEK/ERK signaling cascade activation, which consequently upregulates the expression of multi-drug resistance associated proteins including MDR, MRP, and LRP, eventually conferring chemoresistance in gastric cancer (Ji et al., 2015). MSC-derived exosomes could deliver the contents to cancer cells, and this interaction is responsible for drug resistance. For instance, in breast cancer, MSCs released exosomes contain miR-222/223, entering breast cancer cells (BCCs) to promote the transition into cycling quiescence, which plays a key role in drug evasion. Further study observed that delivering anti-miR-222/223 by antagomiR-loaded MSCs to the dormant BCCs improves the efficiency of carboplatin and then increased host survival (Bliss et al., 2016). Moreover, MSC-exosomes mediated drug resistance has been documented in hematological tumors as well. For example, bone marrow stromal cells (BMSCs) derived exosomes function as a communicator mediating cell-to-cell communication through transference of their contents in multiple myeloma (MM) cells. BMSC-derived exosomes activate several pathways including p38, p53, c-Jun N-terminal kinase, and AKT pathways related to survival, promoting MM cell survival and chemoresistance in vivo by increasing antiapoptotic protein Bcl-2 and reducing the cleavage of caspase-9, caspase-3 (Wang et al., 2014).

Direct Cell-Cell Contact

In addition to releasing paracrine factors and exosomes, MSCs could confer resistance through direct cellular interactions. This cross-talk between cancer cells and MSCs enables to promote the activation of a series of signaling cascades in different tumors (Wang J. et al., 2018). Mudry et al. (2000) has demonstrated that MSCs protect leukemia cells from cytarabine and etoposide cytotoxicity by directly contacting with leukemic cells, thus promoting the expression of vascular cell adhesion molecule-1 (VCAM-1). Further investigations have been done to figure out the detailed protective mechanisms of MSCs adhesion. In T cell acute lymphoblastic leukemia (T-ALL), MSCs adherence to cancer cells, mediated by intercellular adhesion molecule-1 (ICAM-1), is proved to induce mitochondria transfer between MSCs and T-ALL cells, leading to the decrease of mitochondrial intracellular ROS levels in T-ALL cells. It is well accepted that excess ROS is responsible for cell apoptosis, which is one of major mechanisms for chemotherapy (Wang J. et al., 2018). Noteworthily, treating with blocking antibody against ICAM-1 could effectively reduce adhesion between T-ALL cells and MSCs, reducing mitochondrial transfer, thereby restoring chemotherapy sensitivity. Additionally, MSCs protect CML stem/progenitor cells from TKI induced apoptosis by increasing N-Cadherin-mediated adhesion and enhancing transcription of β-catenin target genes in primary CML CD34+ cells. Not surprisingly, the β-catenin inhibitor, ICG001, targeting Wnt signaling enhanced the sensitivity of CML to TKI cocultured with MSC (Zhang et al., 2013).

Aside from hematological malignancies, MSCs are also elucidated to be involved in the drug resistance in solid tumors by direct contact. In oral squamous cell carcinomas (OSCCs), co-cultured with MSCs, the human derived OSCC cell lines are shown activation of PDGF-AA/PDGFR-α autocrine loop, accompanied with the upregulation of AKT, which reduced apoptotic response by increasing expression of Bcl-2 and eventually contributed to cisplatin resistance in OSCC (Wang J. et al., 2020). MSCs co-culture also improves stemness and confers chemo-resistance in gastric cancer (GC) cells by inducing the expression of metabolic pathways related LncRNA histocompatibility leukocyte antigen complex P5 (HCP5) in GC cells. Mechanistically, HCP5 is confirmed to target miR-3619-5p, facilitating FAO by activating AMPK/PGC1α/CEBPB axis to promote stemness and concomitantly mediate chemoresistance in GC cells (Wu et al., 2020).

Genetic Mutations in MSCs

It has long been acknowledged that somatic mutations in tumor cells is a major cause of drug resistance. Some recent studies found genomic alterations also occur in non-malignant cells, which contribute to latent tumor recurrence in patients receiving chemotherapy and radiotherapy (Shi et al., 2017). Patocs et al. (2007) observed genetic mutations in breast cancer stromal cells partly contribute to the poor clinical outcome. In B16F0 melanoma cells, p53-deficient MSCs increase the expression of inducible nitric oxide synthase (iNOS), which is known to be responsible for regulating antitumor immunity and cell survival, leading to vigorous immunosuppression, promoting the facilitation of tumor growth, thus conferring therapy resistance. The inhibition of iNOS could reverse the enhanced tumor-promoting effects of p53-deficient MSCs, suggesting a window of opportunity to target iNOS to restore the sensitivity of MSCs (Huang et al., 2014).

Differentiating Into CAF or CSC

As mentioned before MSCs have the potential to differentiate into multicellular lineages and their conversion to CSCs or CAFs could be another mechanism to confer therapeutic resistance. CSCs have the ability to induce tumor progression and metastasis, and are considered to be inherently resistant to chemotherapy. It has been shown that targeting the methylation of two tumor suppressor gene HIC1 and RassF1A in MSCs induces their differentiating into CSCs and obtaining CSCs characteristics, including the acquisition of drug resistance along with loss of anchorage dependence, increasing colony-forming capacity and pluripotency (Teng et al., 2011). CAFs, as discussed above, play critical role in drug resistance. Some studies have suggested human BM-MSC from healthy donors can transform toward αSMA- and FSP-1-expressing CAFs when exposed to the conditioned medium of tumor cells (Mishra et al., 2008). Dzobo et al. (2016) observed that longer incubation of breast cancer MDAMB 231 cells with human MSCs promotes hMSCs differentiate into CAF, along with the increasing levels of α-SMA and type I collagen, which is mediated by TGF-β/Smad signaling pathway (Senthebane et al., 2017). Further investigation reveals the relation between CAF and MSC in human cancer and their common contribution to drug resistance. Through analyzing human neuroblastoma (NB) tumor, Borriello et al. demonstrated a group of αFAP- and FSP-1-positive CAF cells that harbor similar phenotype and functionality to BM-MSC in the tumor stroma. These cells (designated CAF-MSC) contribute to various steps of tumor development, ranging from enhancing cell proliferation, decreasing cell apoptosis to endowing resistance to chemotherapy. Further study demonstrated that pro-tumorigenic effects mediated by CAF-MSC are associated with the activation of STAT3 and ERK1/2 in NB cells, consistent with IL-6 induced drug resistance mentioned above (Borriello et al., 2017). Hence the inhibition of STAT3 and ERK1/2 may open a new window to enhance the chemotherapy sensitivity.

Based on these multiple mechanisms of MSCs mediated drug resistance (Table 5), targeting the secreting of paracrine factors such as CXCR1/2, CXCL12 and PIFAs is proved to be a novel therapeutic approach (Le Naour et al., 2020; Wang S. et al., 2020). Moreover, due to the multifaceted role of MSCs in tumor progression, MSC-based anti-cancer therapies guide new strategies to overcome therapy resistance. For example, MSCs are being exploited as selective carriers for drug delivery in cancers because of their strong tropism and recruitment to tumors (Li et al., 2021). Several preclinical studies have been conducted to exploit the tumor-targeting ability of MSCs, using MSCs as an excellent in vivo vehicle to deliver tumor-killing drugs (Kim et al., 2015; Yin et al., 2018). Further therapeutic strategy is genetic modification of MSC to overexpress specific immunomodulatory cytokines, suicide genes and other molecules that can effectively inhibit tumor progression, including IFNα, IFNβ and (TNF)-related apoptosis-inducing ligand (TRAIL) (Kidd et al., 2010; Kim et al., 2012). Phase I and Phase II clinical trials of MSC-based anti-cancer therapies are currently in progress (von Einem et al., 2019). In conclusion, an in-depth exploration of the cellular and molecular mechanisms of drug resistance in MSCs is essential to improve existing anticancer therapies.

TABLE 5
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Table 5. Mechanisms of antitumor drug resistance mediated by MSCs.

Cancer Associated Adipocytes

Clinical data have shown epidemiological evidence linking obesity and poor prognosis in cancers at multiple specific sites (Calle et al., 2003). Growing researches highlight the independent effect of obesity to induce resistance to chemotherapies especially in breast cancer, ovarian cancer, prostate cancer, and leukemia (Ewertz et al., 2011), all of which implicate the underlying role of adipocytes in tumor drug resistance. Adipocytes are key components as one of stromal cells in TME (Nieman et al., 2013). It is noteworthy that the bidirectional cross-talk between adipocytes and cancer cells may partly explain cancer progression. Co-cultured with cancer cells, adipocytes are observed to exhibit remarkable phenotypic changes, designated as cancer associated adipocytes (CAAs) (Muller, 2013). And these phenotypic and functional alterations including the delipidation, reduced expression of adipose markers such as Ap2(FABP4), adiponectin and the overexpression of inflammatory cytokines are found to be related to drug resistance (Dirat et al., 2011). Bochet et al. (2013) demonstrated Wnt3a secreted by tumor cells could contribute to the alteration of adipocyte. Emerging evidence indicates that CAAs in TME play dynamic and sophisticated roles in determining resistance to treatments through distinct mechanisms involving regulating metabolism, secreting various factors, altering chemotherapy pharmacokinetics, and remodeling extracellular matrix (Muller, 2013; Choi et al., 2018; Zhang M.M. et al., 2018; Lehuédé et al., 2019).

Regulating Metabolism

Adipocytes were initially identified as a tremendous energy storage providing high-energy metabolites. It is natural to expect a metabolic cross-talk between adipocytes and tumor cells contributing to the progression of tumor cells (Figure 3). The “Warburg effect” and “reverse Warburg effect” have been shown to be responsible for the drug resistance mediated by CAFs, and this concept could be applied to adipocytes as well (Duong et al., 2017). Under hypoxic conditions, lactate released from adipocytes increases dramatically (Pérez de Heredia et al., 2010). Alternatively, accumulating evidence indicates that lipids is the major energy source provided by adipocytes to tumor cells. CAAs release exogenous free fatty acids (FFAs), which are taken up by cancer cells via surface molecule CD36. FFAs could yield large quantity of ATP by increasing the rate of fatty acid β-oxydation (FAO) (Yang et al., 2020), thus contributing to the tumor progression and therapy resistance. In ovarian cancer cells, adipocytes adjust tumor metabolism by upregulating the expression of CD36, which was observed to regulate cellular metabolism including extracellular acidification, intracellular cholesterol accumulation and oxygen consumption, leading to substantial lipid droplets (LDs) accumulation and intracellular reactive oxygen species (ROS) increase (Ladanyi et al., 2018). Growing evidence has indicated that LDs function as organelles influencing chemotherapy response by storing excessive cholesterol and lipids (Guillaumond et al., 2015). Apart from CD36, FATPs (fatty acid transport protein family) and FABPpm (plasma membrane fatty acid binding protein) are reported to facilitate the FA transport process (Zhang M.M. et al., 2018). Likewise, adipocytes induce FABP4 expression, promoting metastasis and mediates carboplatin resistance in ovarian cancer cells. Meanwhile, knockdown of FABP4 leads to increased levels of DNA demethylation, downregulating genetic markers associated with OvCa metastasis and reducing the survival of clonal cancer cell, which provides theoretical support for targeting FABP combined with platinum treatment (Mukherjee et al., 2020).

Secreting Various Factors

It is well acknowledged that aside from the energy storing function, adipose tissue is also a major endocrine organ producing a range of growth factors, adipokines, and adipocytokines, several of which have been demonstrated to confer therapy resistance (Duong et al., 2017).

The generation and secretion of leptin are found to be elevated in CAAs, compared to mature adipocytes. Previous studies have shown the up-regulated leptin could reduce toxicity of chemotherapy agents in vitro through the suppression of intracellular ROS. Further study revealed that adipocytes-derived leptin promotes myeloma cells proliferation and reduces the chemotherapy induced-apoptosis by mediating proliferation and apoptosis related proteins, which is related to the activation of JAK/STAT-PI3K/AKT pathway (Yu et al., 2016). Leptin could bind to the leptin receptor (OB-R), and then contributes to the drug resistance in melanoma cells via activating the PI3K/AKT and MEK/ERK signaling. Interestingly, siRNA knockdown of OB-Rb reverses the activation of AKT and ERK and enhances the chemosensitivity melanoma cells (Chi et al., 2014). Similar finding was reported in colon cancer cells, the combination of leptin and OB-R activates the PI3K/AKT signaling pathway, enhances tumor growth and promotes sphere formation through the overexpression of E-cadherin. Meanwhile, leptin could interfere with the efficacy of the chemotherapeutic agent 5-FU through promoting cell proliferation and suppressing 5-FU-induced apoptosis (Bartucci et al., 2010). In breast cancer cells, leptin participates in resistance to hormonal therapy. Leptin activates the estrogen receptor-alpha (ER-α) through the MAPK pathway regardless of the presence of estradiol, leading to nuclear localization of ER via promoting the expression of pS2, a classic estrogen-dependent gene. Consequently, the estrogen withdrawal status induced by aromatase inhibitors is alleviated, thus contributing to the progression of estrogen-dependent breast cancer (Catalano et al., 2004).

Adipocyte-secreted cytokines have been found to induce resistance via the modulation of cell death. IL-6, IL-8, MCP-1 are the most abundantly adipocyte-secreted cytokines (Duong et al., 2017). Recent studies suggested that increased expression and secretion of IL-6 in CAAs plays a key role in mediating breast cancer progression (Kim et al., 2018). In HER2-positive breast cancers, IL-6 expression can induce CSC-positive phenotype through activating NF-κB and STAT3 pathways, thus driving tumorigenesis and promoting chemotherapy resistance (Liu S. et al., 2018). SDF-1α, another adipocyte-derived chemoattractant, was reported to promote the migration of ALL toward adipose tissue, where leukemia cells could be protected from chemotherapy by remaining in a dormant state, thereby gaining survival advantage (Pramanik et al., 2013).

L-asparaginase (ASNase) is a major treatment regimen for ALL by depleting plasma asparagine and glutamine, while glutamine synthetase was found to be remarkedly elevated in CAAs in ALL. That means adipocytes prevent leukemic cell from ASNase induced cytotoxicity through directly increasing secretion of glutamine (Ehsanipour et al., 2013). Arachidonic acid (AA) is another chemo-protective lipid mediator secreted by adipocytes. It has been shown that AA significantly promotes the resistance of ovarian cancer cells to chemotherapeutic agents, partly dependent on AKT pathway. In addition, AA may participate in the modulation of drug resistance-related cell surface proteins including MRP1 and P-gP, influencing their organization, distribution and activity (Yang et al., 2019). Moreover, adipose-derived factors were demonstrated to confer the inhibition of trastuzumab-mediated ADCC in HER2+ breast tumor cells through decreasing the secretion of INF-γ in natural killer cells without altering their cytotoxicity. Further investigation remains to be done to determine the exact factor (Duong et al., 2015). Additional evidence suggests that adipocyte-derived adipokines activate JAK/STAT3 signaling and induce the upregulation of autophagic proteins, such as Atg5, Atg3, and LC3-I/II, activating autophagy thereby decreasing chemotherapy-induced apoptosis in myeloma cells, which highlights a novel therapeutic target for enhancing chemotherapy sensitivity in myeloma patients (Liu Z.Q. et al., 2015).

In addition to these factors, exosomes derived from CAAs also contribute to drug resistance in tumor cells, as a novel method of transmitting information among cells. Yeung et al. confirmed that CAAs-derived exosomes transfer higher levels of microRNA-21 (miR21) to ovarian cancer cells, which binds to a direct downstream target APAF1, known as a chemoresistance-associated gene, downregulating its expression, leading to paclitaxel resistance. Briefly, adipocytes derived exosomes could promote drug resistance and a malignant phenotype by decreasing the expression of APAF1 in ovarian cancer cells (Yeung et al., 2016).

Altering Chemotherapy Pharmacokinetics

The concentration of active drugs is of particular importance in tumor treatment. However, it was found to be reduced in adipocyte-rich microenvironments, including adipose tissue, omentum, and bone marrow, leading to a localized decrease in the cytotoxic activity of chemotherapy, which partly accounts for chemoresistance (Sheng et al., 2017). Adipocytes alter chemotherapeutic pharmacokinetics mainly through two pathways, including increasing drug clearance and altering drug distribution. Anthracyclines are widely used in a variety of cancers as classical DNA-damaging agents, while adipocytes were demonstrated to highly expressed daunorubicin-metabolizing enzymes, aldo-keto reductases (AKR) and carbonyl reductases (CBR) isoenzymes to deactivate anthracyclines. Specifically, adipocytes reduce the antileukemia effect of daunorubicin by converting it to a less toxic metabolite, thereby reducing active drug concentration in the local microenvironment. Furthermore, Lehuédé et al. (2019) shown the doxorubicin subcellular distribution modified by adipocytes is associated with upregulating major vault protein (MVP). MVP is known as a major component of vault particles, involving in intracellular molecules transportation, including anti-cancer drugs. Therefore, increased expression of MVP in tumor cells induced by adipocytes increases drug efflux and decreases drug intracellular accumulation. Also, it has been demonstrated that overexpression of MVP clinically relates to drug resistance in human breast tumors, indicating a poor prognosis for chemotherapy (Lehuédé et al., 2019).

Extracellular Matrix Remodeling

As previously mentioned, the dynamic adaptation of ECM is essential for cancer progression and invasion as well as drug resistance. Interestingly, adipocytes are vital source of ECM components. In breast tumors, adipocytes increased expression of matrix metalloproteinase-11 (MMP11), along with MMP1, MMP7, MMP10, and MMP14, involving in cisplatin resistance (Satoh et al., 1994; Choi et al., 2018). Collagen VI, another adipocyte-secreted ECM protein was reported to trigger tumor progression in vivo via activation of the NG2 receptor in cancer cells and sequentially inducing Akt, β-catenin, and cyclin D1 (Iyengar et al., 2005). Remarkably, the presence of collagen VI protein was found to promote resistance in cisplatin-sensitive ovarian cells, suggesting that reorganization of the EMC near the tumor is of great importance in drug resistance (Sherman-Baust et al., 2003). Furthermore, a cleavage product of collagen VI, endotrophin highly secreted from adipocytes upon chemotherapy was demonstrated to act as a signaling molecule enhancing EMT process, causing cisplatin resistance. Thiazolidinediones and the neutralization of endotrophin were found to increase chemo-sensitivity by suppressing EMT (Park et al., 2013).

Taken together, the aforementioned studies suggest the complicated role of adipocytes and lipid metabolism in the regulation of anticancer drug sensitivity (Table 6), which makes CAAs targeted therapy a potentially effective treatment. CAAs secrete metabolic substrates, adipokines, and cytokines and promote drug resistance, which may become a potential target for new treatments. For instance, targeting serum IL-6 by tocilizumab, an anti–IL-6 receptor antibody was demonstrated to improve prognosis and alleviate cachexia in chemotherapy-resistant patients with metastatic lung cancer (Ando et al., 2014). In addition, inhibition of CAAs lipolysis provides an opportunity of anticancer therapy. Mechanistically, inhibit the release of FFA and other metabolites from CAAs, thereby constrain the supply of lipid fuel to cancer cells. Alternatively, interference with FFA uptake provide another way to limit FFA supply to tumor cells. Usage of the CD36-neutralizing antibodies to inhibit fatty acid receptor CD36 leads to therapeutically suppression of tumor growth and metastasis in oral squamous cell carcinomas (Pascual et al., 2017). In ovarian cancer, small molecule inhibition of FABP4 diminishes fatty acids transfer and lipid accumulation in cancer cells, impeding intraabdominal metastasis and growth (Nieman et al., 2011). Recent study also demonstrated that BMS309403, a small molecule inhibitor of FABP4, markedly blocks cell proliferation as well as efficiently restores sensitivity of tumor cells to platinum both in vitro and in vivo (Mukherjee et al., 2020). However, it is still challenging to selectively target CAAs without affecting other cells. Therefore, identifying the specific molecular mechanisms of adipocyte-mediated drug resistance can help explore additional targets and develop new ways to combat drug resistance in combination with chemotherapy.

TABLE 6
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Table 6. Mechanisms of antitumor drug resistance mediated by CAAs.

Endothelial Cells

In addition to the cells mentioned above, endothelial cells (ECs), covering the inner surfaces of tumor blood vessels, are yet another vital stroma cells in tumor microenvironment that contribute to drug resistance (Hida et al., 2016). As a key mediator in blood vessel growth, ECs are now regarded as the main target cells for anti-vascular therapy. Cumulative evidence indicates that there is considerable heterogeneity in ECs. Tumor endothelial cells (TECs), a special subpopulation of ECs, are phenotypically and functionally different from normal endothelial cells (NECs), which exhibit the property of being quiescent and proliferate only once every 150 days (Hida et al., 2018). And it is the phenotypic and genotypic heterogeneities of TECs that offer novel mechanisms of resistance (Annan et al., 2020).

Cytogenetic abnormalities, including chromosomal aberration like aneuploidy and abnormal centrosomes, have been observed in TECs isolated from human and murine renal cell carcinoma (Akino et al., 2009; Maishi et al., 2019), suggesting that genetic instability is likely to account for the high frequency of resistance to chemotherapeutic drugs in TECs. TECs isolated from HCC were observed to possess enhanced angiogenic activity and acquire resistance to doxorubicin and 5-fluorouracil (Xiong et al., 2009). In vivo, several studies have elucidated that the expression of multidrug resistance protein 1 gene (MDR1) and its product, p-glycoprotein were increased in TECs compared to NECs, resulting in tumor growth and drug resistance (Huang et al., 2013; Kikuchi et al., 2020). MDR1 (ABCB1), MRP1 (ABCC1), and ABCG2 are all important ABC (ATP-binding cassette) transporters, which are known for conferring multidrug resistance by pumping drugs out of cells, decreasing intracellular drug concentrations (Gottesman et al., 2002). The up-regulation of MDR1 in TECs may be related to AKT activation caused by high level of VEGF secreted from tumor cells, which could be sufficiently impeded by the VEGFR kinase inhibitor, Ki8751 (Akiyama et al., 2012). Chemotherapy induced high IL-8 expression in tumor cells contributes to the upregulation of MDR1 expression in TECs, which in turn causes drug resistance in human bladder cancer cells (Kikuchi et al., 2020). Moreover, some studies showed that TECs express p-glycoprotein and confer resistance to anti-angiogenic drugs (Naito et al., 2016). Accordingly, drugs of P-glycoprotein inhibitor, such as verapamil, suppressed tumor angiogenesis and abrogated TEC resistance, and increased the sensitivity of tumor endothelium to chemotherapeutics (Akiyama et al., 2015; Bani et al., 2017). In a word, the high expression of P-glycoprotein and other ABC transporters in TECs plays a vital role in mediating multidrug resistance (Figure 3).

Hyperglycolytic metabolism has been noted as another major character of TECs versus NECs. The RNA sequencing of TECs and NECs revealed that the expression of most glycolytic genes are up-regulated in TECs, such as PFKFB3, encoding glucose transporter GLUT1 (Slc2a1). And this altered glycolytic metabolism is involved in the formation of abnormal tumor vessels, thus rendering chemoresistance by impairing the delivery and efficacy of chemotherapy. Targeting PFKFB3 in ECs, rather than angiogenic signals, to modulate ECs’ metabolism is an effective way to promote tumor vessel normalization (TVN), with increased chemotherapy sensitivity (Cantelmo et al., 2016).

The stemness properties of TECs was claimed to be responsible for resistance to anticancer drugs as well. It has been elucidated that TECs express stem cell markers including the ABC transporter, MDR1, as demonstrated above (Annan et al., 2020). Besides, aldehyde metabolism associated enzyme, namely aldehyde dehydrogenase (ALDH), is considered to be a stem cell marker in TECs. Hida et al. (2017) demonstrated that the increased ALDHhigh TECs population induced by tumor-secreting factors in TME were accompanied by upregulation of stem-related genes such as MDR1, CD90, ALP, and Oct-4. That may be the cause of resistance to drug therapy.

Tavora et al. (2014) described that TEC-derived focal adhesion kinase (FAK) contributes to the acquisition of chemoresistance, via regulating DNA-damaging related NF-κB pathway and enhancing the subsequent production of cytokines from endothelial cells in vivo and vitro. Additionally, endothelial-cell FAK deficiency is sufficient to restore the sensitivity of tumor cells to DNA-damaging therapies through decreasing the activation of NF-κB and the following cytokine production. In consistence, the work is supported by clinical relevance as well. In lymphoma patients, disease progression is found to be correlated with altered endothelial cell FAK expression (Tavora et al., 2014).

Endothelial cells-derived paracrine factors, angiocrine factors, are highlighted in conferring drug resistance by the network of endothelial-carcinoma signaling interactions. Tumor-necrosis factor-α (TNF-α), an essential upstream activator of the NF-κB signaling cascade, was found to be strikingly upregulated in adjacent endothelial cells in breast cancer after doxorubicin chemotherapy treatment (Acharyya et al., 2012), which was induced by the overexpression of CXCL1/2 in breast cancer cells and S100A8/9 in CD11b+Gr1+ myeloid cells. Moreover, NF-κB activation amplified the CXCL1/2-S100A8/9 loop in turn. As a result, the highly activation of TNF-α-CXCL1/2-S100A8/9 paracrine network drives chemoresistance by activating ERK1/2, p38 MAPK, and p70S6K, mediating the pro-survival effect in tumor cells. Fibroblast growth factor (FGF) 4, originated from B cell lymphoma cells (LCs), was reported to activate FGFR1, which upregulated the expression of Notch ligand Jagged1 (Jag1) on neighboring ECs. Reciprocally, the elevated EC-derived angiocrine Jag1 promotes LC chemoresistance by activating Notch2–Hey1 signals in LCs. In brief, these results suggested the importance of FGF4-FGFR1/Jag1-Notch2 loop between LCs and ECs in fostering chemoresistance. Obviously angiocrine Jag1 is central to this loop and inhibiting the FGF4/Jag1 feed-forward signaling loop between LCs and ECs could sensitize LCs to chemotherapeutics such as doxorubicin (Cao et al., 2014). Furthermore, the importance of Notch signaling in drug resistance has been proven in other tumors. Hoarau-Vechot et al. (2019) demonstrated that AKT-activated ECs increase the expression of Jagged 1, activating notch signaling and inducing chemoresistance in ovarian cancer. Clinically, high Notch3 expression is notably associated with poorer overall survival and enhanced drug resistance. Thus, targeting of aberrant NOTCH signaling plays a critical role in suppressing ECs-mediated pro-tumoral niche in combination with other therapeutic strategies. IL-6, a proinflammatory cytokine increasingly secreted by other stroma cells, is an important angiocrine factor secreted by TECs as well. Bent et al. (2016) showed that strong expression of IL-6 from ECs was mediated by ROS-induced p38 activation in vitro under doxorubicin treatment. In consequence, IL-6 represses senescence-associated inflammation, promoting chemoresistance via the suppression of PI3K/AKT/mTOR pathway in B-cell lymphoma. Additionally, insulin growth factor (IGF) binding protein-7 (IGFBP7/angiomodulin), an important tumor-suppressive checkpoint expressed by TEC, was reported to participate in the TEC angiocrine mediated chemoresistance as well. Tumor derived FGF4 activates FGFR1 in endothelial cells and stimulates EST-2-dependent upregulation of IGF1 and suppression of IGFBP7, leading to chemotherapy tolerance and promoting tumor recurrence and lethality (Cao et al., 2017).

Moreover, it has been shown that ECs play an important part in mediating resistance to anti-vascular drugs and immunotherapy (Nagl et al., 2020). In glioblastoma, tumor derived PDGF activates ECs, inducing NF-κB-dependent Snail expression, resulting in endothelial-mesenchymal transformation (Endo-MT). Further, Endo-MT abrogates the expression of VEGFR-2, the major regulator of angiogenesis, causing endothelial resistance to anti-VEGF treatment (Liu T. et al., 2018). Remarkably, PDGFR-β knockout in ECs robustly sensitizes GBM tumors to anti-VEGF therapy, suggesting targeting PDGF/NF-κB/Snail axis and preventing Endo-MT in ECs may offer exciting opportunities in antiangiogenic therapy resistance. In addition to encasing blood vessels, endothelial cells also form the inner layer of lymphatic vessels, which implicates ECs also involve in treatment response to checkpoint antibody therapy as key mediators of immune regulation (Nagl et al., 2020). By detecting 1,592 endothelial cells in lung cancer, Lambrechts et al. (2018) revealed that TECs downregulate immune attraction pathways by reducing the expression of chemotaxis (CCL2, CCL18, and IL6), adhesion molecules (ICAM1) and antigen presentation associated molecular (major histocompatibility complex class I and II), which contributes to tumor immunotolerance in TME. Besides, TECs promote the formation of abnormal tumor vessels, which facilitates the presence of immunosuppressive immune cells, attenuating the efficacy of immunotherapy based on immune checkpoint inhibitors (ICIs) (Schaaf et al., 2018).

As discussed above, ECs induce resistance to chemotherapy, anti-vascular therapy, and immunotherapy through multiple mechanisms, including cytogenetic abnormalities, hyperglycolytic metabolism, secreting paracrine factors and inducing abnormal tumor vasculature (Table 7). Hence, targeting these crosstalks and signaling axis as stated before can help overcome tolerogenic events. In particular, reprogramming the ECs glycolytic phenotype and promoting tumor vasculature-normalizing, combined with immunotherapy are promising strategy (Stapor et al., 2014; Cantelmo et al., 2016).

TABLE 7
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Table 7. Mechanisms of antitumor drug resistance mediated by ECs.

Platelets

Derived from common hematopoietic progenitor cells, platelet is a key regulator in hemostasis and thrombosis (Contursi et al., 2017). However, emerging studies have focused on its contributions to various aspects of cancer progression, including angiogenesis, tumor growth, metastasis and drug resistance (D’Alessandro et al., 2015; Tesfamariam, 2016; Contursi et al., 2017). Multiple reports have shown a strong link between platelets and the efficiency of tumor chemotherapy. For instance, platelet-sparing phenomenon was reported in patients treated with carboplatin and paclitaxel chemotherapy (Pertusini et al., 2001). Moreover, differential platelet levels or the platelet/lymphocyte ratios have been suggested to be a potential predictive factor of chemotherapy response or survival prognosis in various tumors, including breast cancer, gastric cancer, NSCLC, pancreatic neuroendocrine tumor, ovarian cancer and so on (Bottsford-Miller et al., 2015; Cuello-López et al., 2018; Fang et al., 2018; Gong et al., 2018; Xu S.S. et al., 2019). Tumor-educated platelets (TEPs) are even considered to be potential non-invasive biomarker in achieving effective cancer management (In ’t Veld and Wurdinger, 2019). Clinically, high platelet count has been correlated with chemotherapy resistance. Therefore, it is necessary to understand the association between platelets and drug-resistance in TME.

Platelets contribute to drug resistance through secreting various factors, altering chemotherapy pharmacokinetics, and eliciting multiple signaling pathways (Table 8).

TABLE 8
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Table 8. Mechanisms of antitumor drug resistance mediated by platelets.

Many reports have indicated platelets to be an important source of diverse growth factors and cytokines, leading to drug resistance in TME (Assoian et al., 1983). As mentioned earlier, TGF-β/NF-κB signaling is a vital pathway involved in tumor drug resistance. Recent experiment demonstrated that platelets not only function as the major source of TGF-β but also express the cell surface-docking receptor glycoprotein A repetitions predominant (GARP), increasing the active TGF-β levels. The GARP-TGF-β axis promoted by platelets constrain T cell immunity against cancer, thus rendering resistance to therapy (Rachidi et al., 2017). Besides, platelet-derived TGF-β could activate the TGF-β/Smad and NF-κB pathways, subsequently leading to the EMT in tumor cells (Labelle et al., 2011), which was suggested to significantly contribute to the development of chemoresistance (Fischer et al., 2015). In pancreatic cancer, TGF-β released by platelets diminished cisplatin sensitivity through activating PI3K/Akt and MEK/Erk signaling (Chen et al., 2013). Apart from TGF-β, other platelet factors were reported to mediate drug resistance in vitro as well. Clusterin, thrombospondin-1, and RANTES secreted by platelet are demonstrated to protect adenocarcinoma cells from anticancer drugs via modulating cancer cell cycle, DNA damage repair pathways and MAPK levels (Radziwon-Balicka et al., 2012).

Another important mechanism lies in modulating drug metabolism. Clinical studies have shown the association of multidrug resistance-associated protein 1 (MRP1) expression and platelet count with clinical outcome in 427 operable NSCLC patients (Wang Z. et al., 2018). In fact, the expression of two ABC transporter in platelets, MRP4 and MRP1, was suggested to be relatively high (Köck et al., 2007), which confers drug resistance by promoting drug efflux, reducing intracellular drug concentrations (Oevermann et al., 2009).

In addition to chemotherapy drugs, platelets can also lead to tolerance to anti-angiogenic therapy. In HCC, platelets derived growth factors such as PDGF, TGF-α, and -β, EGF and serotonin, are ascribed to modulate the sensitivity and resistance to multikinase inhibitors (D’Alessandro et al., 2015). In glioblastoma multiforme (GBM) patients, platelet-derived VEGF shows potent pro-angiogenic effects on GBM-derived endothelial cells. Patients with GBM have significantly higher intraplatelet VEGF concentrations compared to healthy controls (Di Vito et al., 2017). Consistently, it has been accepted that redundancy of vascular stimulation signals may be the basis for resistance to anti-angiogenic therapy (van Beijnum et al., 2015).

Accordingly, in terms of platelet-induced drug resistance, apart from targeting relevant platelet-originated factors (e.g., PDGF, TGFβ1, and EGF) and pathways including TGF-β/NF-κB signaling, targeting the activity of platelets in TME is an important approach to improve the sensitivity of tumor therapy. Aspirin, a potent inhibitor of platelet function, has been suggested to potentially enhance the sensitivity to 5-Fu-based chemotherapy in colorectal cancer (CRC) via abrogating the activation of NF-κB both in vivo and in vitro (Fu et al., 2019). Ticagrelor, an inhibitor of the ADP–P2Y12 axis, was demonstrated to boost chemotherapeutic efficacy synergized with chemotherapeutic agents in pancreatic cancer cells, which was mediated by reducing EGF-dependent AKT activation (Elaskalani et al., 2020). Noteworthily, potential challenges remain in antiplatelet strategies during cancer therapy, including the risk of bleeding and comorbidity. Further experimental and clinical confirmation validation are warranted to validate the benefits and risks of combined antiplatelet therapy in cancer patients.

Conclusion

Taken together, the evidence we summarized here clearly demonstrate that TME has a considerable impact on tumorigenesis and resistance in the context of therapeutic intervention. Therefore, TME is an attractive target for both sensitizing tumors to traditional therapies and as an alternative choice for resistant disease. Targeting these stroma cells is a potentially helpful adjunct to immunotherapy and targeted therapy. Repolarization and normalization rather than elimination of these cells seems a preferable choice. Despite of the heat of immunotherapy, we cannot ignore the fact that chemotherapies and molecular targeted therapies are still basic and effective in many cancers, especially for early-stage patients. The primary challenges lie in that we need to determine the best combinations or sequences and manage patients based on whether they are likely to benefit from a specific drug or drug combination.

In any case, our current insight into the cancer therapy suggests that rapid tumor cell elimination is crucial to prevent acquired therapeutic resistance. In order to achieve this goal, treatment combinations need to be optimized to delay the progression of drug resistance. Meanwhile, novel strategies targeting and reshaping the microenvironment to block pro-tumor cross-talk and restore immune surveillance are urgently required. Lastly, because current preclinical models of TME cannot completely represent variations exhibited by patients of different histological types, detailed molecular and cellular profiles are needed for clinical trials, which is necessary for identifying predictive biomarkers and promoting the development of personalized treatment.

Author Contributions

YN and XTZ contributed to the first draft of the article, the tables, and the figures. JY provided assistance in making figures. HS and HL revised the manuscript. XZ and XM conceived the presented idea, revised the manuscript again, and approved the final version. All authors approved the manuscript for publication.

Funding

This work was supported by the Funding of Sichuan Provincial Science and Technology Department (No. 2018JY0165), the National Major Scientific and Technological Special Project for the “Significant New Drugs Development” (No. 2018ZX09201018-013), the National Natural Science Foundation of China (No. 81821002), the National Science and Technology Major Projects for Major New Drugs Innovation and Development (No. 2018ZX09733001-004), and the National Natural Science Foundation of China (No. 81902662).

Conflict of Interest

The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest.

References

Acharyya, S., Oskarsson, T., Vanharanta, S., Malladi, S., Kim, J., Morris, P. G., et al. (2012). A CXCL1 paracrine network links cancer chemoresistance and metastasis. Cell 150, 165–178. doi: 10.1016/j.cell.2012.04.042

PubMed Abstract | CrossRef Full Text | Google Scholar

Adamo, A., Dal Collo, G., Bazzoni, R., and Krampera, M. (2019). Role of mesenchymal stromal cell-derived extracellular vesicles in tumour microenvironment. Biochim. Biophys. Acta Rev. Cancer 1871, 192–198. doi: 10.1016/j.bbcan.2018.12.001

PubMed Abstract | CrossRef Full Text | Google Scholar

Aggen, D. H., Ager, C. R., Obradovic, A. Z., Chowdhury, N., Ghasemzadeh, A., Mao, W., et al. (2021). Blocking IL1 beta promotes tumor regression and remodeling of the myeloid compartment in a renal cell carcinoma model: multidimensional analyses. Clin. Cancer Res. 27, 608–621. doi: 10.1158/1078-0432.CCR-20-1610

PubMed Abstract | CrossRef Full Text | Google Scholar

Akino, T., Hida, K., Hida, Y., Tsuchiya, K., Freedman, D., Muraki, C., et al. (2009). Cytogenetic abnormalities of tumor-associated endothelial cells in human malignant tumors. Am. J. Pathol. 175, 2657–2667. doi: 10.2353/ajpath.2009.090202

PubMed Abstract | CrossRef Full Text | Google Scholar

Akiyama, K., Maishi, N., Ohga, N., Hida, Y., Ohba, Y., Alam, M. T., et al. (2015). Inhibition of multidrug transporter in tumor endothelial cells enhances antiangiogenic effects of low-dose metronomic paclitaxel. Am. J. Pathol. 185, 572–580. doi: 10.1016/j.ajpath.2014.10.017

PubMed Abstract | CrossRef Full Text | Google Scholar

Akiyama, K., Ohga, N., Hida, Y., Kawamoto, T., Sadamoto, Y., Ishikawa, S., et al. (2012). Tumor endothelial cells acquire drug resistance by MDR1 up-regulation via VEGF signaling in tumor microenvironment. Am. J. Pathol. 180, 1283–1293. doi: 10.1016/j.ajpath.2011.11.029

PubMed Abstract | CrossRef Full Text | Google Scholar

Akkari, L., Bowman, R. L., Tessier, J., Klemm, F., Handgraaf, S. M., de Groot, M., et al. (2020). Dynamic changes in glioma macrophage populations after radiotherapy reveal CSF-1R inhibition as a strategy to overcome resistance. Sci. Transl. Med. 12:eaaw7843. doi: 10.1126/scitranslmed.aaw7843

PubMed Abstract | CrossRef Full Text | Google Scholar

Allen, E., Miéville, P., Warren, C. M., Saghafinia, S., Li, L., Peng, M. W., et al. (2016). Metabolic symbiosis enables adaptive resistance to anti-angiogenic therapy that is dependent on mtor signaling. Cell Rep. 15, 1144–1160. doi: 10.1016/j.celrep.2016.04.029

PubMed Abstract | CrossRef Full Text | Google Scholar

Amawi, H., Sim, H. M., Tiwari, A. K., Ambudkar, S. V., and Shukla, S. (2019). ABC transporter-mediated multidrug-resistant cancer. Adv. Exp. Med. Biol. 1141, 549–580. doi: 10.1007/978-981-13-7647-4_12

CrossRef Full Text | Google Scholar

Ambrose, J., Livitz, M., Wessels, D., Kuhl, S., Lusche, D. F., Scherer, A., et al. (2015). Mediated coalescence: a possible mechanism for tumor cellular heterogeneity. Am. J. Cancer Res. 5, 3485–3504.

Google Scholar

Ando, K., Takahashi, F., Kato, M., Kaneko, N., Doi, T., Ohe, Y., et al. (2014). Tocilizumab, a proposed therapy for the cachexia of Interleukin6-expressing lung cancer. PLoS One 9:e102436. doi: 10.1371/journal.pone.0102436

PubMed Abstract | CrossRef Full Text | Google Scholar

Angst, E., Reber, H. A., Hines, O. J., and Eibl, G. (2008). Mononuclear cell-derived interleukin-1 beta confers chemoresistance in pancreatic cancer cells by upregulation of cyclooxygenase-2. Surgery 144, 57–65. doi: 10.1016/j.surg.2008.03.024

PubMed Abstract | CrossRef Full Text | Google Scholar

Annan, D. A., Kikuchi, H., Maishi, N., Hida, Y., and Hida, K. (2020). Tumor endothelial cell-a biological tool for translational cancer research. Int. J. Mol. Sci. 21:3238. doi: 10.3390/ijms21093238

PubMed Abstract | CrossRef Full Text | Google Scholar

Apicella, M., Giannoni, E., Fiore, S., Ferrari, K. J., Fernández-Pérez, D., Isella, C., et al. (2018). Increased lactate secretion by cancer cells sustains non-cell-autonomous adaptive resistance to MET and EGFR targeted therapies. Cell Metab. 28, 848.e6–865.e6. doi: 10.1016/j.cmet.2018.08.006

PubMed Abstract | CrossRef Full Text | Google Scholar

Aslan, K., Turco, V., Blobner, J., Sonner, J. K., Liuzzi, A. R., Núñez, N. G., et al. (2020). Heterogeneity of response to immune checkpoint blockade in hypermutated experimental gliomas. Nat. Commun. 11:931. doi: 10.1038/s41467-020-14642-0

PubMed Abstract | CrossRef Full Text | Google Scholar

Assoian, R. K., Komoriya, A., Meyers, C. A., Miller, D. M., and Sporn, M. B. (1983). Transforming growth factor-beta in human platelets. Identification of a major storage site, purification, and characterization. J. Biol. Chem. 258, 7155–7160.

Google Scholar

Baghdadi, M., Wada, H., Nakanishi, S., Abe, H., Han, N., Putra, W. E., et al. (2016). Chemotherapy-Induced IL34 enhances immunosuppression by tumor-associated macrophages and mediates survival of chemoresistant lung cancer cells. Cancer Res. 76, 6030–6042. doi: 10.1158/0008-5472.Can-16-1170

PubMed Abstract | CrossRef Full Text | Google Scholar

Bamias, A., Koutsoukou, V., Terpos, E., Tsiatas, M. L., Liakos, C., Tsitsilonis, O., et al. (2008). Correlation of NK T-like CD3+CD56+ cells and CD4+CD25+(hi) regulatory T cells with VEGF and TNFalpha in ascites from advanced ovarian cancer: association with platinum resistance and prognosis in patients receiving first-line, platinum-based chemotherapy. Gynecol. Oncol. 108, 421–427. doi: 10.1016/j.ygyno.2007.10.018

PubMed Abstract | CrossRef Full Text | Google Scholar

Bani, M., Decio, A., Giavazzi, R., and Ghilardi, C. (2017). Contribution of tumor endothelial cells to drug resistance: anti-angiogenic tyrosine kinase inhibitors act as p-glycoprotein antagonists. Angiogenesis 20, 233–241. doi: 10.1007/s10456-017-9549-6

PubMed Abstract | CrossRef Full Text | Google Scholar

Bartucci, M., Svensson, S., Ricci-Vitiani, L., Dattilo, R., Biffoni, M., Signore, M., et al. (2010). Obesity hormone leptin induces growth and interferes with the cytotoxic effects of 5-fluorouracil in colorectal tumor stem cells. Endocr. Relat. Cancer 17, 823–833. doi: 10.1677/ERC-10-0083

PubMed Abstract | CrossRef Full Text | Google Scholar

Bedke, J., Albiges, L., Capitanio, U., Giles, R. H., Hora, M., Lam, T. B., et al. (2021). Updated European Association of urology guidelines on renal cell carcinoma: nivolumab plus cabozantinib joins immune checkpoint inhibition combination therapies for treatment-naïve metastatic clear-cell renal cell carcinoma. Eur. Urol. 79, 339–342. doi: 10.1016/j.eururo.2020.12.005

PubMed Abstract | CrossRef Full Text | Google Scholar

Bent, E. H., Gilbert, L. A., and Hemann, M. T. (2016). A senescence secretory switch mediated by PI3K/AKT/mTOR activation controls chemoprotective endothelial secretory responses. Genes Dev. 30, 1811–1821. doi: 10.1101/gad.284851.116

PubMed Abstract | CrossRef Full Text | Google Scholar

Binenbaum, Y., Fridman, E., Yaari, Z., Milman, N., Schroeder, A., Ben David, G., et al. (2018). Transfer of miRNA in macrophage-derived exosomes induces drug resistance in pancreatic adenocarcinoma. Cancer Res. 78, 5287–5299. doi: 10.1158/0008-5472.Can-18-0124

PubMed Abstract | CrossRef Full Text | Google Scholar

Bliss, S. A., Sinha, G., Sandiford, O. A., Williams, L. M., Engelberth, D. J., Guiro, K., et al. (2016). Mesenchymal stem cell-derived exosomes stimulate cycling quiescence and early breast cancer dormancy in bone marrow. Cancer Res. 76, 5832–5844. doi: 10.1158/0008-5472.Can-16-1092

PubMed Abstract | CrossRef Full Text | Google Scholar

Bochet, L., Lehuédé, C., Dauvillier, S., Wang, Y. Y., Dirat, B., Laurent, V., et al. (2013). Adipocyte-derived fibroblasts promote tumor progression and contribute to the desmoplastic reaction in breast cancer. Cancer Res. 73, 5657–5668. doi: 10.1158/0008-5472.Can-13-0530

PubMed Abstract | CrossRef Full Text | Google Scholar

Borriello, L., Nakata, R., Sheard, M. A., Fernandez, G. E., Sposto, R., Malvar, J., et al. (2017). Cancer-associated fibroblasts share characteristics and protumorigenic activity with mesenchymal stromal cells. Cancer Res. 77, 5142–5157. doi: 10.1158/0008-5472.CAN-16-2586

PubMed Abstract | CrossRef Full Text | Google Scholar

Bottsford-Miller, J., Choi, H. J., Dalton, H. J., Stone, R. L., Cho, M. S., Haemmerle, M., et al. (2015). Differential platelet levels affect response to taxane-based therapy in ovarian cancer. Clin. Cancer Res. 21, 602–610. doi: 10.1158/1078-0432.Ccr-14-0870

PubMed Abstract | CrossRef Full Text | Google Scholar

Calcinotto, A., Spataro, C., Zagato, E., Di Mitri, D., Gil, V., Crespo, M., et al. (2018). IL-23 secreted by myeloid cells drives castration-resistant prostate cancer. Nature 559, 363–369. doi: 10.1038/s41586-018-0266-0

PubMed Abstract | CrossRef Full Text | Google Scholar

Calle, E. E., Rodriguez, C., Walker-Thurmond, K., and Thun, M. J. (2003). Overweight, obesity, and mortality from cancer in a prospectively studied cohort of US adults. N. Engl. J. Med. 348, 1625–1638. doi: 10.1056/NEJMoa021423

PubMed Abstract | CrossRef Full Text | Google Scholar

Campbell, J. R., McDonald, B. R., Mesko, P. B., Siemers, N. O., Singh, P. B., Selby, M., et al. (2021). Fc-optimized Anti-CCR8 antibody depletes regulatory T cells in human tumor models. Cancer Res. doi: 10.1158/0008-5472.Can-20-3585 [Epub ahead of print].

CrossRef Full Text | PubMed Abstract | Google Scholar

Cantelmo, A. R., Conradi, L. C., Brajic, A., Goveia, J., Kalucka, J., Pircher, A., et al. (2016). Inhibition of the glycolytic activator PFKFB3 in endothelium induces tumor vessel normalization, impairs metastasis, and improves chemotherapy. Cancer Cell 30, 968–985. doi: 10.1016/j.ccell.2016.10.006

PubMed Abstract | CrossRef Full Text | Google Scholar

Cao, Z., Ding, B. S., Guo, P., Lee, S. B., Butler, J. M., Casey, S. C., et al. (2014). Angiocrine factors deployed by tumor vascular niche induce B cell lymphoma invasiveness and chemoresistance. Cancer Cell 25, 350–365. doi: 10.1016/j.ccr.2014.02.005

PubMed Abstract | CrossRef Full Text | Google Scholar

Cao, Z., Scandura, J. M., Inghirami, G. G., Shido, K., Ding, B. S., and Rafii, S. (2017). Molecular checkpoint decisions made by subverted vascular niche transform indolent tumor cells into chemoresistant cancer stem cells. Cancer Cell 31, 110–126. doi: 10.1016/j.ccell.2016.11.010

PubMed Abstract | CrossRef Full Text | Google Scholar

Cardenas, H., Vieth, E., Lee, J., Segar, M., Liu, Y., Nephew, K. P., et al. (2014). TGF-β induces global changes in DNA methylation during the epithelial-to-mesenchymal transition in ovarian cancer cells. Epigenetics 9, 1461–1472. doi: 10.4161/15592294.2014.971608

PubMed Abstract | CrossRef Full Text | Google Scholar

Catalano, S., Mauro, L., Marsico, S., Giordano, C., Rizza, P., Rago, V., et al. (2004). Leptin induces, via ERK1/ERK2 signal, functional activation of estrogen receptor alpha in MCF-7 cells. J. Biol. Chem. 279, 19908–19915. doi: 10.1074/jbc.M313191200

PubMed Abstract | CrossRef Full Text | Google Scholar

Cazet, A. S., Hui, M. N., Elsworth, B. L., Wu, S. Z., Roden, D., Chan, C. L., et al. (2018). Targeting stromal remodeling and cancer stem cell plasticity overcomes chemoresistance in triple negative breast cancer. Nat. Commun. 9:2897. doi: 10.1038/s41467-018-05220-6

PubMed Abstract | CrossRef Full Text | Google Scholar

Che, Y., Wang, J., Li, Y., Lu, Z., Huang, J., Sun, S., et al. (2018). Cisplatin-activated PAI-1 secretion in the cancer-associated fibroblasts with paracrine effects promoting esophageal squamous cell carcinoma progression and causing chemoresistance. Cell Death Dis. 9:759. doi: 10.1038/s41419-018-0808-2

PubMed Abstract | CrossRef Full Text | Google Scholar

Chen, H., Lan, X., Liu, M., Zhou, B., Wang, B., and Chen, P. (2013). Direct TGF-β1 signaling between activated platelets and pancreatic cancer cells primes cisplatin insensitivity. Cell Biol. Int. 37, 478–484. doi: 10.1002/cbin.10067

PubMed Abstract | CrossRef Full Text | Google Scholar

Chi, M., Chen, J., Ye, Y., Tseng, H. Y., Lai, F., Tay, K. H., et al. (2014). Adipocytes contribute to resistance of human melanoma cells to chemotherapy and targeted therapy. Curr. Med. Chem. 21, 1255–1267. doi: 10.2174/0929867321666131129114742

PubMed Abstract | CrossRef Full Text | Google Scholar

Choi, J., Cha, Y. J., and Koo, J. S. (2018). Adipocyte biology in breast cancer: from silent bystander to active facilitator. Prog. Lipid Res. 69, 11–20. doi: 10.1016/j.plipres.2017.11.002

PubMed Abstract | CrossRef Full Text | Google Scholar

Ciardiello, D., Elez, E., Tabernero, J., and Seoane, J. (2020). Clinical development of therapies targeting TGFβ: current knowledge and future perspectives. Ann. Oncol. 31, 1336–1349. doi: 10.1016/j.annonc.2020.07.009

PubMed Abstract | CrossRef Full Text | Google Scholar

Contursi, A., Sacco, A., Grande, R., Dovizio, M., and Patrignani, P. (2017). Platelets as crucial partners for tumor metastasis: from mechanistic aspects to pharmacological targeting. Cell Mol. Life Sci. 74, 3491–3507. doi: 10.1007/s00018-017-2536-7

PubMed Abstract | CrossRef Full Text | Google Scholar

Cuello-López, J., Fidalgo-Zapata, A., López-Agudelo, L., and Vásquez-Trespalacios, E. (2018). Platelet-to-lymphocyte ratio as a predictive factor of complete pathologic response to neoadjuvant chemotherapy in breast cancer. PLoS One 13:e0207224. doi: 10.1371/journal.pone.0207224

PubMed Abstract | CrossRef Full Text | Google Scholar

D’Alessandro, R., Messa, C., Refolo, M. G., and Carr, B. I. (2015). Modulation of sensitivity and resistance to multikinase inhibitors by microenvironmental platelet factors in HCC. Expert Opin. Pharmacother. 16, 2773–2780. doi: 10.1517/14656566.2015.1101065

PubMed Abstract | CrossRef Full Text | Google Scholar

De Henau, O., Rausch, M., Winkler, D., Campesato, L. F., Liu, C., Cymerman, D. H., et al. (2016). Overcoming resistance to checkpoint blockade therapy by targeting PI3Kγ in myeloid cells. Nature 539, 443–447. doi: 10.1038/nature20554

PubMed Abstract | CrossRef Full Text | Google Scholar

De Veirman, K., Menu, E., Maes, K., De Beule, N., De Smedt, E., Maes, A., et al. (2019). Myeloid-derived suppressor cells induce multiple myeloma cell survival by activating the AMPK pathway. Cancer Lett. 442, 233–241. doi: 10.1016/j.canlet.2018.11.002

PubMed Abstract | CrossRef Full Text | Google Scholar

Deaglio, S., Dwyer, K. M., Gao, W., Friedman, D., Usheva, A., Erat, A., et al. (2007). Adenosine generation catalyzed by CD39 and CD73 expressed on regulatory T cells mediates immune suppression. J. Exp. Med. 204, 1257–1265. doi: 10.1084/jem.20062512

PubMed Abstract | CrossRef Full Text | Google Scholar

Deng, X., Ruan, H., Zhang, X., Xu, X., Zhu, Y., Peng, H., et al. (2020). Long noncoding RNA CCAL transferred from fibroblasts by exosomes promotes chemoresistance of colorectal cancer cells. Int. J. Cancer 146, 1700–1716. doi: 10.1002/ijc.32608

PubMed Abstract | CrossRef Full Text | Google Scholar

Deying, W., Feng, G., Shumei, L., Hui, Z., Ming, L., and Hongqing, W. (2017). CAF-derived HGF promotes cell proliferation and drug resistance by up-regulating the c-Met/PI3K/Akt and GRP78 signalling in ovarian cancer cells. Biosci. Rep. 37:BSR20160470. doi: 10.1042/bsr20160470

PubMed Abstract | CrossRef Full Text | Google Scholar

Di Vito, C., Navone, S. E., Marfia, G., Abdel Hadi, L., Mancuso, M. E., Pecci, A., et al. (2017). Platelets from glioblastoma patients promote angiogenesis of tumor endothelial cells and exhibit increased VEGF content and release. Platelets 28, 585–594. doi: 10.1080/09537104.2016.1247208

PubMed Abstract | CrossRef Full Text | Google Scholar

Diggs, L. P., Ruf, B., Ma, C., Heinrich, B., Cui, L., Zhang, Q., et al. (2020). CD40-mediated immune cell activation enhances response to anti-PD-1 in murine intrahepatic cholangiocarcinoma. J. Hepatol. 74, 1145–1154. doi: 10.1016/j.jhep.2020.11.037

PubMed Abstract | CrossRef Full Text | Google Scholar

Dirat, B., Bochet, L., Dabek, M., Daviaud, D., Dauvillier, S., Majed, B., et al. (2011). Cancer-associated adipocytes exhibit an activated phenotype and contribute to breast cancer invasion. Cancer Res. 71, 2455–2465. doi: 10.1158/0008-5472.Can-10-3323

PubMed Abstract | CrossRef Full Text | Google Scholar

Doi, T., Muro, K., Ishii, H., Kato, T., Tsushima, T., Takenoyama, M., et al. (2019). A Phase I study of the Anti-CC Chemokine Receptor 4 antibody, mogamulizumab, in combination with nivolumab in patients with advanced or metastatic solid tumors. Clin. Cancer Res. 25, 6614–6622. doi: 10.1158/1078-0432.Ccr-19-1090

PubMed Abstract | CrossRef Full Text | Google Scholar

Duong, M. N., Cleret, A., Matera, E. L., Chettab, K., Mathe, D., Valsesia-Wittmann, S., et al. (2015). Adipose cells promote resistance of breast cancer cells to trastuzumab-mediated antibody-dependent cellular cytotoxicity. Breast Cancer Res. 17:57. doi: 10.1186/s13058-015-0569-0

PubMed Abstract | CrossRef Full Text | Google Scholar

Duong, M. N., Geneste, A., Fallone, F., Li, X., Dumontet, C., and Muller, C. (2017). The fat and the bad: mature adipocytes, key actors in tumor progression and resistance. Oncotarget 8, 57622–57641. doi: 10.18632/oncotarget.18038

PubMed Abstract | CrossRef Full Text | Google Scholar

Dzobo, K., Vogelsang, M., Thomford, N. E., Dandara, C., Kallmeyer, K., Pepper, M. S., et al. (2016). Wharton’s jelly-derived mesenchymal stromal cells and fibroblast-derived extracellular matrix synergistically activate apoptosis in a p21-dependent mechanism in WHCO1 and MDA MB 231 cancer cells in vitro. Stem Cells Int. 2016:4842134. doi: 10.1155/2016/4842134

PubMed Abstract | CrossRef Full Text | Google Scholar

Ebbing, E. A., van der Zalm, A. P., Steins, A., Creemers, A., Hermsen, S., Rentenaar, R., et al. (2019). Stromal-derived interleukin 6 drives epithelial-to-mesenchymal transition and therapy resistance in esophageal adenocarcinoma. Proc. Natl. Acad. Sci. U.S.A. 116, 2237–2242. doi: 10.1073/pnas.1820459116

PubMed Abstract | CrossRef Full Text | Google Scholar

Ehsanipour, E. A., Sheng, X., Behan, J. W., Wang, X. C., Butturini, A., Avramis, V. I., et al. (2013). Adipocytes cause leukemia cell resistance to L-Asparaginase via release of glutamine. Cancer Res. 73, 2998–3006. doi: 10.1158/0008-5472.Can-12-4402

PubMed Abstract | CrossRef Full Text | Google Scholar

Elaskalani, O., Domenichini, A., Abdol Razak, N. B., Dye D, E., Falasca, M., and Metharom, P. (2020). Antiplatelet drug ticagrelor enhances chemotherapeutic efficacy by targeting the novel P2Y12-AKT pathway in pancreatic cancer cells. Cancers 12:250. doi: 10.3390/cancers12010250

PubMed Abstract | CrossRef Full Text | Google Scholar

Ewertz, M., Jensen, M. B., Gunnarsdottir, K. A., Hojris, I., Jakobsen, E. H., Nielsen, D., et al. (2011). Effect of obesity on prognosis after early-stage breast cancer. J. Clin. Oncol. 29, 25–31. doi: 10.1200/JCO.2010.29.7614

PubMed Abstract | CrossRef Full Text | Google Scholar

Fang, L., Sheng, H., Wan, D., Zhu, C., Jiang, R., Sun, X., et al. (2018). Prognostic role of multidrug resistance-associated protein 1 expression and platelet count in operable non-small cell lung cancer. Oncol. Lett. 16, 1123–1132. doi: 10.3892/ol.2018.8763

PubMed Abstract | CrossRef Full Text | Google Scholar

Fang, Y., Zhou, W., Rong, Y., Kuang, T., Xu, X., Wu, W., et al. (2019). Exosomal miRNA-106b from cancer-associated fibroblast promotes gemcitabine resistance in pancreatic cancer. Exp. Cell Res. 383:111543. doi: 10.1016/j.yexcr.2019.111543

PubMed Abstract | CrossRef Full Text | Google Scholar

Fiori, M. E., Di Franco, S., Villanova, L., Bianca, P., Stassi, G., and De Maria, R. (2019). Cancer-associated fibroblasts as abettors of tumor progression at the crossroads of EMT and therapy resistance. Mol. Cancer 18:70. doi: 10.1186/s12943-019-0994-2

PubMed Abstract | CrossRef Full Text | Google Scholar

Fischer, K. R., Durrans, A., Lee, S., Sheng, J., Li, F., Wong, S. T., et al. (2015). Epithelial-to-mesenchymal transition is not required for lung metastasis but contributes to chemoresistance. Nature 527, 472–476. doi: 10.1038/nature15748

PubMed Abstract | CrossRef Full Text | Google Scholar

Folgiero, V., Miele, E., Carai, A., Ferretti, E., Alfano, V., Po, A., et al. (2016). IDO1 involvement in mTOR pathway: a molecular mechanism of resistance to mTOR targeting in medulloblastoma. Oncotarget 7, 52900–52911. doi: 10.18632/oncotarget.9284

PubMed Abstract | CrossRef Full Text | Google Scholar

Fridlender, Z. G., Sun, J., Kim, S., Kapoor, V., Cheng, G., Ling, L., et al. (2009). Polarization of tumor-associated neutrophil phenotype by TGF-beta: “N1” versus “N2”. TAN. Cancer Cell 16, 183–194. doi: 10.1016/j.ccr.2009.06.017

PubMed Abstract | CrossRef Full Text | Google Scholar

Fu, H., Yang, H., Zhang, X., and Xu, W. (2016). The emerging roles of exosomes in tumor-stroma interaction. J. Cancer Res. Clin. Oncol. 142, 1897–1907. doi: 10.1007/s00432-016-2145-0

PubMed Abstract | CrossRef Full Text | Google Scholar

Fu, J., Xu, Y., Yang, Y., Liu, Y., Ma, L., and Zhang, Y. (2019). Aspirin suppresses chemoresistance and enhances antitumor activity of 5-Fu in 5-Fu-resistant colorectal cancer by abolishing 5-Fu-induced NF-κB activation. Scie. Rep. 9:16937. doi: 10.1038/s41598-019-53276-1

PubMed Abstract | CrossRef Full Text | Google Scholar

Fultang, L., Panetti, S., Ng, M., Collins, P., Graef, S., Rizkalla, N., et al. (2019). MDSC targeting with Gemtuzumab ozogamicin restores T cell immunity and immunotherapy against cancers. EBioMedicine 47, 235–246. doi: 10.1016/j.ebiom.2019.08.025

PubMed Abstract | CrossRef Full Text | Google Scholar

Gabrilovich, D. I. (2017). Myeloid-derived suppressor cells. Cancer Immunol. Res. 5, 3–8. doi: 10.1158/2326-6066.Cir-16-0297

PubMed Abstract | CrossRef Full Text | Google Scholar

Gilbert, P. M., Havenstrite, K. L., Magnusson, K. E., Sacco, A., Leonardi, N. A., Kraft, P., et al. (2010). Substrate elasticity regulates skeletal muscle stem cell self-renewal in culture. Science 329, 1078–1081. doi: 10.1126/science.1191035

PubMed Abstract | CrossRef Full Text | Google Scholar

Gong, W., Zhao, L., Dong, Z., Dou, Y., Liu, Y., Ma, C., et al. (2018). After neoadjuvant chemotherapy platelet/lymphocyte ratios negatively correlate with prognosis in gastric cancer patients. J. Clin. Lab. Anal. 32:e22364. doi: 10.1002/jcla.22364

PubMed Abstract | CrossRef Full Text | Google Scholar

Gottesman, M. M., Fojo, T., and Bates, S. E. (2002). Multidrug resistance in cancer: role of ATP-dependent transporters. Nat. Rev. Cancer 2, 48–58. doi: 10.1038/nrc706

PubMed Abstract | CrossRef Full Text | Google Scholar

Gourdin, N., Bossennec, M., Rodriguez, C., Vigano, S., Machon, C., Jandus, C., et al. (2018). Autocrine adenosine regulates tumor polyfunctional CD73(+)CD4(+) effector T Cells devoid of immune checkpoints. Cancer Res. 78, 3604–3618. doi: 10.1158/0008-5472.Can-17-2405

PubMed Abstract | CrossRef Full Text | Google Scholar

Guillaumond, F., Bidaut, G., Ouaissi, M., Servais, S., Gouirand, V., Olivares, O., et al. (2015). Cholesterol uptake disruption, in association with chemotherapy, is a promising combined metabolic therapy for pancreatic adenocarcinoma. Proc. Natl. Acad. Sci. U.S.A. 112, 2473–2478. doi: 10.1073/pnas.1421601112

PubMed Abstract | CrossRef Full Text | Google Scholar

Guillén Díaz-Maroto, N., Sanz-Pamplona, R., Berdiel-Acer, M., Cimas, F. J., García, E., Gonçalves-Ribeiro, S., et al. (2019). Noncanonical TGFβ pathway relieves the blockade of IL1β/TGFβ-Mediated crosstalk between tumor and stroma: TGFBR1 and TAK1 inhibition in colorectal cancer. Clin. Cancer Res. 25, 4466–4479. doi: 10.1158/1078-0432.CCR-18-3957

PubMed Abstract | CrossRef Full Text | Google Scholar

Guo, Q. R., Wang, H., Yan, Y. D., Liu, Y., Su, C. Y., Chen, H. B., et al. (2020). The role of exosomal microRNA in cancer drug resistance. Front. Oncol. 10:472. doi: 10.3389/fonc.2020.00472

PubMed Abstract | CrossRef Full Text | Google Scholar

Gyori, D., Lim, E. L., Grant, F. M., Spensberger, D., Roychoudhuri, R., Shuttleworth, S. J., et al. (2018). Compensation between CSF1R+ macrophages and Foxp3+ Treg cells drives resistance to tumor immunotherapy. JCI Insight 3:e120631. doi: 10.1172/jci.insight.120631

PubMed Abstract | CrossRef Full Text | Google Scholar

Halbrook, C. J., Pontious, C., Kovalenko, I., Lapienyte, L., Dreyer, S., Lee, H. J., et al. (2019). Macrophage-released pyrimidines inhibit gemcitabine therapy in pancreatic Cancer. Cell Metab. 29, 1390.e6–1399.e6. doi: 10.1016/j.cmet.2019.02.001

PubMed Abstract | CrossRef Full Text | Google Scholar

Han, Z. P., Jing, Y. Y., Xia, Y., Zhang, S. S., Hou, J., Meng, Y., et al. (2014). Mesenchymal stem cells contribute to the chemoresistance of hepatocellular carcinoma cells in inflammatory environment by inducing autophagy. Cell Biosci. 4:22. doi: 10.1186/2045-3701-4-22

PubMed Abstract | CrossRef Full Text | Google Scholar

Hanahan, D., and Weinberg, R. A. (2011). Hallmarks of cancer: the next generation. Cell 144, 646–674. doi: 10.1016/j.cell.2011.02.013

PubMed Abstract | CrossRef Full Text | Google Scholar

Hanson, J. A., Gillespie, J. W., Grover, A., Tangrea, M. A., Chuaqui, R. F., Emmert-Buck, M. R., et al. (2006). Gene promoter methylation in prostate tumor-associated stromal cells. J. Natl. Cancer Inst. 98, 255–261. doi: 10.1093/jnci/djj051

PubMed Abstract | CrossRef Full Text | Google Scholar

He, W., Liang, B., Wang, C., Li, S., Zhao, Y., Huang, Q., et al. (2019). MSC-regulated lncRNA MACC1-AS1 promotes stemness and chemoresistance through fatty acid oxidation in gastric cancer. Oncogene 38, 4637–4654. doi: 10.1038/s41388-019-0747-0

PubMed Abstract | CrossRef Full Text | Google Scholar

Hida, K., Maishi, N., Akiyama, K., Ohmura-Kakutani, H., Torii, C., Ohga, N., et al. (2017). Tumor endothelial cells with high aldehyde dehydrogenase activity show drug resistance. Cancer Sci. 108, 2195–2203. doi: 10.1111/cas.13388

PubMed Abstract | CrossRef Full Text | Google Scholar

Hida, K., Maishi, N., Annan, D. A., and Hida, Y. (2018). Contribution of tumor endothelial cells in cancer progression. Int. J. Mol. Sci. 19:1272. doi: 10.3390/ijms19051272

PubMed Abstract | CrossRef Full Text | Google Scholar

Hida, K., Maishi, N., Sakurai, Y., Hida, Y., and Harashima, H. (2016). Heterogeneity of tumor endothelial cells and drug delivery. Adv. Drug Deliv. Rev. 99(Pt B), 140–147. doi: 10.1016/j.addr.2015.11.008

PubMed Abstract | CrossRef Full Text | Google Scholar

Hientz, K., Mohr, A., Bhakta-Guha, D., and Efferth, T. (2017). The role of p53 in cancer drug resistance and targeted chemotherapy. Oncotarget 8, 8921–8946. doi: 10.18632/oncotarget.13475

PubMed Abstract | CrossRef Full Text | Google Scholar

Hirata, E., Girotti, M. R., Viros, A., Hooper, S., Spencer-Dene, B., Matsuda, M., et al. (2015). Intravital imaging reveals how BRAF inhibition generates drug-tolerant microenvironments with high integrin β1/FAK signaling. Cancer Cell 27, 574–588. doi: 10.1016/j.ccell.2015.03.008

PubMed Abstract | CrossRef Full Text | Google Scholar

Hoarau-Vechot, J., Touboul, C., Halabi, N., Blot-Dupin, M., Lis, R., Abi Khalil, C., et al. (2019). Akt-activated endothelium promotes ovarian cancer proliferation through notch activation. J. Transl. Med. 17:194. doi: 10.1186/s12967-019-1942-z

PubMed Abstract | CrossRef Full Text | Google Scholar

Holmgaard, R. B., Zamarin, D., Lesokhin, A., Merghoub, T., and Wolchok, J. D. (2016). Targeting myeloid-derived suppressor cells with colony stimulating factor-1 receptor blockade can reverse immune resistance to immunotherapy in indoleamine 2,3-dioxygenase-expressing tumors. EBioMedicine 6, 50–58. doi: 10.1016/j.ebiom.2016.02.024

PubMed Abstract | CrossRef Full Text | Google Scholar

Hu, J. L., Wang, W., Lan, X. L., Zeng, Z. C., Liang, Y. S., Yan, Y. R., et al. (2019). CAFs secreted exosomes promote metastasis and chemotherapy resistance by enhancing cell stemness and epithelial-mesenchymal transition in colorectal cancer. Mol. Cancer 18:91. doi: 10.1186/s12943-019-1019-x

PubMed Abstract | CrossRef Full Text | Google Scholar

Huang, H., Wang, C., Liu, F., Li, H. Z., Peng, G., Gao, X., et al. (2018). Reciprocal network between cancer stem-like cells and macrophages facilitates the progression rogen deprivation therapy resistance of prostate Cancer. Clin. Cancer Res. 24, 4612–4626. doi: 10.1158/1078-0432.Ccr-18-0461

PubMed Abstract | CrossRef Full Text | Google Scholar

Huang, L., Perrault, C., Coelho-Martins, J., Hu, C., Dulong, C., Varna, M., et al. (2013). Induction of acquired drug resistance in endothelial cells and its involvement in anticancer therapy. J. Hematol. Oncol. 6:49. doi: 10.1186/1756-8722-6-49

PubMed Abstract | CrossRef Full Text | Google Scholar

Huang, W. C., Kuo, K. T., Wang, C. H., Yeh, C. T., and Wang, Y. (2019). Cisplatin resistant lung cancer cells promoted M2 polarization of tumor-associated macrophages via the Src/CD155/MIF functional pathway. J. Exp. Clin. Cancer Res. 38:180. doi: 10.1186/s13046-019-1166-3

PubMed Abstract | CrossRef Full Text | Google Scholar

Huang, Y., Yu, P., Li, W., Ren, G., Roberts, A. I., Cao, W., et al. (2014). p53 regulates mesenchymal stem cell-mediated tumor suppression in a tumor microenvironment through immune modulation. Oncogene 33, 3830–3838. doi: 10.1038/onc.2013.355

PubMed Abstract | CrossRef Full Text | Google Scholar

Hui, L., and Chen, Y. (2015). Tumor microenvironment: sanctuary of the devil. Cancer Lett. 368, 7–13. doi: 10.1016/j.canlet.2015.07.039

PubMed Abstract | CrossRef Full Text | Google Scholar

Imbert, C., Montfort, A., Fraisse, M., Marcheteau, E., Gilhodes, J., Martin, E., et al. (2020). Resistance of melanoma to immune checkpoint inhibitors is overcome by targeting the sphingosine kinase-1. Nat. Commun. 11:437. doi: 10.1038/s41467-019-14218-7

PubMed Abstract | CrossRef Full Text | Google Scholar

In ’t Veld, S., and Wurdinger, T. (2019). Tumor-educated platelets. Blood 133, 2359–2364. doi: 10.1182/blood-2018-12-852830

PubMed Abstract | CrossRef Full Text | Google Scholar

Incio, J., Liu, H., Suboj, P., Chin, S. M., Chen, I. X., Pinter, M., et al. (2016). Obesity-induced inflammation and desmoplasia promote pancreatic cancer progression and resistance to chemotherapy. Cancer Discov. 6, 852–869. doi: 10.1158/2159-8290.Cd-15-1177

PubMed Abstract | CrossRef Full Text | Google Scholar

Iyengar, P., Espina, V., Williams, T. W., Lin, Y., Berry, D., Jelicks, L. A., et al. (2005). Adipocyte-derived collagen VI affects early mammary tumor progression in vivo, demonstrating a critical interaction in the tumor/stroma microenvironment. J. Clin. Invest. 115, 1163–1176. doi: 10.1172/jci23424

PubMed Abstract | CrossRef Full Text | Google Scholar

Jacobetz, M. A., Chan, D. S., Neesse, A., Bapiro, T. E., Cook, N., Frese, K. K., et al. (2013). Hyaluronan impairs vascular function and drug delivery in a mouse model of pancreatic cancer. Gut 62, 112–120. doi: 10.1136/gutjnl-2012-302529

PubMed Abstract | CrossRef Full Text | Google Scholar

Ji, R. B., Zhang, B., Zhang, X., Xue, J. G., Yuan, X., Yan, Y. M., et al. (2015). Exosomes derived from human mesenchymal stem cells confer drug resistance in gastric cancer. Cell Cycle 14, 2473–2483. doi: 10.1080/15384101.2015.1005530

PubMed Abstract | CrossRef Full Text | Google Scholar

Jiménez-Valerio, G., Martínez-Lozano, M., Bassani, N., Vidal, A., Ochoa-de-Olza, M., Suárez, C., et al. (2016). Resistance to antiangiogenic therapies by metabolic symbiosis in renal cell carcinoma PDX models and patients. Cell Rep. 15, 1134–1143. doi: 10.1016/j.celrep.2016.04.015

PubMed Abstract | CrossRef Full Text | Google Scholar

Jinushi, M., Chiba, S., Yoshiyama, H., Masutomi, K., Kinoshita, I., Dosaka-Akita, H., et al. (2011). Tumor-associated macrophages regulate tumorigenicity and anticancer drug responses of cancer stem/initiating cells. Proc. Natl. Acad. Sci. U.S.A. 108, 12425–12430. doi: 10.1073/pnas.1106645108

PubMed Abstract | CrossRef Full Text | Google Scholar

Johansson, A. C., Ansell, A., Jerhammar, F., Lindh, M. B., Grénman, R., Munck-Wikland, E., et al. (2012). Cancer-associated fibroblasts induce matrix metalloproteinase-mediated cetuximab resistance in head and neck squamous cell carcinoma cells. Mol. Cancer Res. 10, 1158–1168. doi: 10.1158/1541-7786.Mcr-12-0030

PubMed Abstract | CrossRef Full Text | Google Scholar

Kalbasi, A., Komar, C., Tooker, G. M., Liu, M., Lee, J. W., Gladney, W. L., et al. (2017). Tumor-Derived CCL2 mediates resistance to radiotherapy in pancreatic ductal adenocarcinoma. Clin. Cancer Res. 23, 137–148. doi: 10.1158/1078-0432.Ccr-16-0870

PubMed Abstract | CrossRef Full Text | Google Scholar

Kalluri, R. (2016). The biology and function of fibroblasts in cancer. Nat. Rev. Cancer 16, 582–598. doi: 10.1038/nrc.2016.73

PubMed Abstract | CrossRef Full Text | Google Scholar

Kalluri, R., and Neilson, E. G. (2003). Epithelial-mesenchymal transition and its implications for fibrosis. J. Clin. Invest. 112, 1776–1784. doi: 10.1172/jci20530

PubMed Abstract | CrossRef Full Text | Google Scholar

Kasahara, K., Arao, T., Sakai, K., Matsumoto, K., Sakai, A., Kimura, H., et al. (2010). Impact of serum hepatocyte growth factor on treatment response to epidermal growth factor receptor tyrosine kinase inhibitors in patients with non-small cell lung adenocarcinoma. Clin. Cancer Res. 16, 4616–4624. doi: 10.1158/1078-0432.Ccr-10-0383

PubMed Abstract | CrossRef Full Text | Google Scholar

Kawano, M., Mabuchi, S., Matsumoto, Y., Sasano, T., Takahashi, R., Kuroda, H., et al. (2015). The significance of G-CSF expression and myeloid-derived suppressor cells in the chemoresistance of uterine cervical cancer. Sci. Rep. 5:18217. doi: 10.1038/srep18217

PubMed Abstract | CrossRef Full Text | Google Scholar

Kidd, S., Caldwell, L., Dietrich, M., Samudio, I., Spaeth, E. L., Watson, K., et al. (2010). Mesenchymal stromal cells alone or expressing interferon-beta suppress pancreatic tumors in vivo, an effect countered by anti-inflammatory treatment. Cytotherapy 12, 615–625. doi: 10.3109/14653241003631815

PubMed Abstract | CrossRef Full Text | Google Scholar

Kikuchi, H., Maishi, N., Annan, D. A., Alam, M. T., Dawood, R. I. H., Sato, M., et al. (2020). Chemotherapy-Induced IL8 Upregulates MDR1/ABCB1 in tumor blood vessels and results in unfavorable outcome. Cancer Res. 80, 2996–3008. doi: 10.1158/0008-5472.CAN-19-3791

PubMed Abstract | CrossRef Full Text | Google Scholar

Kim, H. S., Jung, M., Choi, S. K., Woo, J., Piao, Y. J., Hwang, E. H., et al. (2018). IL-6-mediated cross-talk between human preadipocytes and ductal carcinoma in situ in breast cancer progression. J. Exp. Clin. Cancer Res. 37:200. doi: 10.1186/s13046-018-0867-3

PubMed Abstract | CrossRef Full Text | Google Scholar

Kim, J., Hall, R. R., Lesniak, M. S., and Ahmed, A. U. (2015). Stem cell-based cell carrier for targeted oncolytic virotherapy: translational opportunity and open questions. Viruses 7, 6200–6217. doi: 10.3390/v7122921

PubMed Abstract | CrossRef Full Text | Google Scholar

Kim, S. M., Woo, J. S., Jeong, C. H., Ryu, C. H., Lim, J. Y., and Jeun, S. S. (2012). Effective combination therapy for malignant glioma with TRAIL-secreting mesenchymal stem cells and lipoxygenase inhibitor MK886. Cancer Res. 72, 4807–4817. doi: 10.1158/0008-5472.Can-12-0123

PubMed Abstract | CrossRef Full Text | Google Scholar

Köck, K., Grube, M., Jedlitschky, G., Oevermann, L., Siegmund, W., Ritter, C. A., et al. (2007). Expression of adenosine triphosphate-binding cassette (ABC) drug transporters in peripheral blood cells: relevance for physiology and pharmacotherapy. Clin. Pharmacokinet. 46, 449–470. doi: 10.2165/00003088-200746060-00001

PubMed Abstract | CrossRef Full Text | Google Scholar

Kodet, O., Dvoøřánková, B., Bendlová, B., Sýkorová, V., Krajsová, I., Štork, J., et al. (2018). Microenvironment-driven resistance to B-Raf inhibition in a melanoma patient is accompanied by broad changes of gene methylation and expression in distal fibroblasts. Int. J. Mol. Med. 41, 2687–2703. doi: 10.3892/ijmm.2018.3448

PubMed Abstract | CrossRef Full Text | Google Scholar

Korbecki, J., Grochans, S., Gutowska, I., Barczak, K., and Baranowska-Bosiacka, I. (2020). CC Chemokines in a tumor: a review of pro-cancer and anti-cancer properties of receptors CCR5, CCR6, CCR7, CCR8, CCR9, and CCR10 Ligands. Int. J. Mol. Sci. 21:7619. doi: 10.3390/ijms21207619

PubMed Abstract | CrossRef Full Text | Google Scholar

Kurose, K., Ohue, Y., Wada, H., Iida, S., Ishida, T., Kojima, T., et al. (2015). Phase ia study of FoxP3+ CD4 treg depletion by infusion of a humanized Anti-CCR4 Antibody, KW-0761, in Cancer Patients. Clin. Cancer Res. 21, 4327–4336. doi: 10.1158/1078-0432.Ccr-15-0357

PubMed Abstract | CrossRef Full Text | Google Scholar

Kuwada, K., Kagawa, S., Yoshida, R., Sakamoto, S., Ito, A., Watanabe, M., et al. (2018). The epithelial-to-mesenchymal transition induced by tumor-associated macrophages confers chemoresistance in peritoneally disseminated pancreatic cancer. J. Exp. Clin. Cancer Res. 37:307. doi: 10.1186/s13046-018-0981-2

PubMed Abstract | CrossRef Full Text | Google Scholar

Labelle, M., Begum, S., and Hynes, R. O. (2011). Direct signaling between platelets and cancer cells induces an epithelial-mesenchymal-like transition and promotes metastasis. Cancer Cell 20, 576–590. doi: 10.1016/j.ccr.2011.09.009

PubMed Abstract | CrossRef Full Text | Google Scholar

Ladanyi, A., Mukherjee, A., Kenny, H. A., Johnson, A., Mitra, A. K., Sundaresan, S., et al. (2018). Adipocyte-induced CD36 expression drives ovarian cancer progression and metastasis. Oncogene 37, 2285–2301. doi: 10.1038/s41388-017-0093-z

PubMed Abstract | CrossRef Full Text | Google Scholar

Lamberti, M. J., Rettel, M., Krijgsveld, J., Rivarola, V. A., and Rumie Vittar, N. B. (2019). Secretome profiling of heterotypic spheroids suggests a role of fibroblasts in HIF-1 pathway modulation and colorectal cancer photodynamic resistance. Cell Oncol. 42, 173–196. doi: 10.1007/s13402-018-00418-8

PubMed Abstract | CrossRef Full Text | Google Scholar

Lambrechts, D., Wauters, E., Boeckx, B., Aibar, S., Nittner, D., Burton, O., et al. (2018). Phenotype molding of stromal cells in the lung tumor microenvironment. Nat. Med. 24, 1277–1289. doi: 10.1038/s41591-018-0096-5

PubMed Abstract | CrossRef Full Text | Google Scholar

Lancet, J. E., Moseley, A. B., Coutre, S. E., DeAngelo, D. J., Othus, M., Tallman, M. S., et al. (2020). A phase 2 study of ATRA, arsenic trioxide, and gemtuzumab ozogamicin in patients with high-risk APL (SWOG 0535). Blood Adv. 4, 1683–1689. doi: 10.1182/bloodadvances.2019001278

PubMed Abstract | CrossRef Full Text | Google Scholar

Le Naour, A., Prat, M., Thibault, B., Mevel, R., Lemaitre, L., Leray, H., et al. (2020). Tumor cells educate mesenchymal stromal cells to release chemoprotective and immunomodulatory factors. J. Mol. Cell Biol. 12, 202–215. doi: 10.1093/jmcb/mjz090

PubMed Abstract | CrossRef Full Text | Google Scholar

Lehuédé, C., Li, X., Dauvillier, S., Vaysse, C., Franchet, C., Clement, E., et al. (2019). Adipocytes promote breast cancer resistance to chemotherapy, a process amplified by obesity: role of the major vault protein (MVP). Breast Cancer Res. 21:7. doi: 10.1186/s13058-018-1088-6

PubMed Abstract | CrossRef Full Text | Google Scholar

Leung, C. S., Yeung, T. L., Yip, K. P., Wong, K. K., Ho, S. Y., Mangala, L. S., et al. (2018). Cancer-associated fibroblasts regulate endothelial adhesion protein LPP to promote ovarian cancer chemoresistance. J. Clin. Invest. 128, 589–606. doi: 10.1172/jci95200

PubMed Abstract | CrossRef Full Text | Google Scholar

Li, C., Yang, W., Gai, X., Zhang, Y., Li, Y., and Fu, H. (2012). Foxp3 overexpression decreases sensitivity to chemotherapy in mouse Lewis lung cancer cells. Mol. Med. Rep. 6, 977–982. doi: 10.3892/mmr.2012.1066

PubMed Abstract | CrossRef Full Text | Google Scholar

Li, C., Zhao, H., and Wang, B. (2021). Mesenchymal stem/stromal cells: developmental origin, tumorigenesis and translational cancer therapeutics. Transl. Oncol. 14:100948. doi: 10.1016/j.tranon.2020.100948

PubMed Abstract | CrossRef Full Text | Google Scholar

Li, I., and Nabet, B. Y. (2019). Exosomes in the tumor microenvironment as mediators of cancer therapy resistance. Mol. Cancer 18, 32. doi: 10.1186/s12943-019-0975-5

PubMed Abstract | CrossRef Full Text | Google Scholar

Li, J., Guan, J., Long, X., Wang, Y., and Xiang, X. (2016). mir-1-mediated paracrine effect of cancer-associated fibroblasts on lung cancer cell proliferation and chemoresistance. Oncol. Rep. 35, 3523–3531. doi: 10.3892/or.2016.4714

PubMed Abstract | CrossRef Full Text | Google Scholar

Li, S., Liu, M., Do, M. H., Chou, C., Stamatiades, E. G., Nixon, B. G., et al. (2020). Cancer immunotherapy via targeted TGF-β signalling blockade in T(H) cells. Nature 587, 121–125. doi: 10.1038/s41586-020-2850-3

PubMed Abstract | CrossRef Full Text | Google Scholar

Li, X., Liu, R., Su, X., Pan, Y., Han, X., Shao, C., et al. (2019). Harnessing tumor-associated macrophages as aids for cancer immunotherapy. Mol. Cancer 18:177. doi: 10.1186/s12943-019-1102-3

PubMed Abstract | CrossRef Full Text | Google Scholar

Li, Z., Chan, K., Qi, Y., Lu, L., Ning, F., Wu, M., et al. (2018). Participation of CCL1 in snail-positive fibroblasts in colorectal cancer contribute to 5-Fluorouracil/Paclitaxel chemoresistance. Cancer Res. Treat. 50, 894–907. doi: 10.4143/crt.2017.356

PubMed Abstract | CrossRef Full Text | Google Scholar

Lis, R., Touboul, C., Mirshahi, P., Ali, F., Mathew, S., Nolan, D. J., et al. (2011). Tumor associated mesenchymal stem cells protects ovarian cancer cells from hyperthermia through CXCL12. Int. J. Cancer 128, 715–725. doi: 10.1002/ijc.25619

PubMed Abstract | CrossRef Full Text | Google Scholar

Liu, H., Wang, J., Zhang, M., Xuan, Q., Wang, Z., Lian, X., et al. (2017). Jagged1 promotes aromatase inhibitor resistance by modulating tumor-associated macrophage differentiation in breast cancer patients. Breast Cancer Res. Treat. 166, 95–107. doi: 10.1007/s10549-017-4394-2

PubMed Abstract | CrossRef Full Text | Google Scholar

Liu, M., Zhou, J., Chen, Z., and Cheng, A. S. (2017). Understanding the epigenetic regulation of tumours and their microenvironments: opportunities and problems for epigenetic therapy. J. Pathol. 241, 10–24. doi: 10.1002/path.4832

PubMed Abstract | CrossRef Full Text | Google Scholar

Liu, S., Lee, J. S., Jie, C., Park, M. H., Iwakura, Y., Patel, Y., et al. (2018). HER2 overexpression triggers an IL1α proinflammatory circuit to drive tumorigenesis and promote chemotherapy resistance. Cancer Res. 78, 2040–2051. doi: 10.1158/0008-5472.Can-17-2761

PubMed Abstract | CrossRef Full Text | Google Scholar

Liu, T., Ma, W., Xu, H., Huang, M., Zhang, D., He, Z., et al. (2018). PDGF-mediated mesenchymal transformation renders endothelial resistance to anti-VEGF treatment in glioblastoma. Nat. Commun. 9:3439. doi: 10.1038/s41467-018-05982-z

PubMed Abstract | CrossRef Full Text | Google Scholar

Liu, X. D., Hoang, A., Zhou, L., Kalra, S., Yetil, A., Sun, M., et al. (2015). Resistance to antiangiogenic therapy is associated with an immunosuppressive tumor microenvironment in metastatic renal cell carcinoma. Cancer Immunol. Res. 3, 1017–1029. doi: 10.1158/2326-6066.Cir-14-0244

PubMed Abstract | CrossRef Full Text | Google Scholar

Liu, Y., and Cao, X. (2015). The origin and function of tumor-associated macrophages. Cell Mol. Immunol. 12, 1–4. doi: 10.1038/cmi.2014.83

PubMed Abstract | CrossRef Full Text | Google Scholar

Liu, Z., Xu, J., He, J., Liu, H., Lin, P., Wan, X., et al. (2015). Mature adipocytes in bone marrow protect myeloma cells against chemotherapy through autophagy activation. Oncotarget 6, 34329–34341.

Google Scholar

Liu, Z. Q., Xu, J. D., He, J., Liu, H., Lin, P., Wan, X. H., et al. (2015). Mature adipocytes in bone marrow protect myeloma cells against chemotherapy through autophagy activation. Oncotarget 6, 34329–34341. doi: 10.18632/oncotarget.6020

PubMed Abstract | CrossRef Full Text | Google Scholar

Long, Y., Tao, H., Karachi, A., Grippin, A. J., Jin, L., Chang, Y. E., et al. (2020). Dysregulation of glutamate transport enhances treg function that promotes VEGF blockade resistance in glioblastoma. Cancer Res. 80, 499–509. doi: 10.1158/0008-5472.Can-19-1577

PubMed Abstract | CrossRef Full Text | Google Scholar

Lu, M., Xie, K., Lu, X., Lu, L., Shi, Y., and Tang, Y. (2020). Notoginsenoside R1 counteracts mesenchymal stem cell-evoked oncogenesis and doxorubicin resistance in osteosarcoma cells by blocking IL-6 secretion-induced JAK2/STAT3 signaling. Invest. New Drugs 39, 416–425. doi: 10.1007/s10637-020-01027-9

PubMed Abstract | CrossRef Full Text | Google Scholar

Luo, J., Lee, S. O., Liang, L., Huang, C. K., Li, L., Wen, S., et al. (2014). Infiltrating bone marrow mesenchymal stem cells increase prostate cancer stem cell population and metastatic ability via secreting cytokines to suppress androgen receptor signaling. Oncogene 33, 2768–2778. doi: 10.1038/onc.2013.233

PubMed Abstract | CrossRef Full Text | Google Scholar

Ma, J., Song, X., Xu, X., and Mou, Y. (2019). Cancer-associated fibroblasts promote the chemo-resistance in gastric cancer through secreting IL-11 Targeting JAK/STAT3/Bcl2 pathway. Cancer Res. Treat. 51, 194–210. doi: 10.4143/crt.2018.031

PubMed Abstract | CrossRef Full Text | Google Scholar

Maishi, N., Annan, D. A., Kikuchi, H., Hida, Y., and Hida, K. (2019). Tumor endothelial heterogeneity in cancer progression. Cancers 11:1511. doi: 10.3390/cancers11101511

PubMed Abstract | CrossRef Full Text | Google Scholar

Makker, V., Rasco, D., Vogelzang, N. J., Brose, M. S., Cohn, A. L., Mier, J., et al. (2019). Lenvatinib plus pembrolizumab in patients with advanced endometrial cancer: an interim analysis of a multicentre, open-label, single-arm, phase 2 trial. Lancet Oncol. 20, 711–718. doi: 10.1016/S1470-2045(19)30020-8

CrossRef Full Text | Google Scholar

Mao, Y., Zhang, Y., Qu, Q., Zhao, M., Lou, Y., Liu, J., et al. (2015). Cancer-associated fibroblasts induce trastuzumab resistance in HER2 positive breast cancer cells. Mol. Biosyst. 11, 1029–1040. doi: 10.1039/c4mb00710g

PubMed Abstract | CrossRef Full Text | Google Scholar

Mathot, P., Grandin, M., Devailly, G., Souaze, F., Cahais, V., Moran, S., et al. (2017). DNA methylation signal has a major role in the response of human breast cancer cells to the microenvironment. Oncogenesis 6:e390. doi: 10.1038/oncsis.2017.88

PubMed Abstract | CrossRef Full Text | Google Scholar

Migneco, G., Whitaker-Menezes, D., Chiavarina, B., Castello-Cros, R., Pavlides, S., Pestell, R. G., et al. (2010). Glycolytic cancer associated fibroblasts promote breast cancer tumor growth, without a measurable increase in angiogenesis: evidence for stromal-epithelial metabolic coupling. Cell Cycle 9, 2412–2422. doi: 10.4161/cc.9.12.11989

PubMed Abstract | CrossRef Full Text | Google Scholar

Mishra, P. J., Mishra, P. J., Humeniuk, R., Medina, D. J., Alexe, G., Mesirov, J. P., et al. (2008). Carcinoma-associated fibroblast-like differentiation of human mesenchymal stem cells. Cancer Res. 68, 4331–4339. doi: 10.1158/0008-5472.CAN-08-0943

PubMed Abstract | CrossRef Full Text | Google Scholar

Mishra, R., Haldar, S., Placencio, V., Madhav, A., Rohena-Rivera, K., Agarwal, P., et al. (2018). Stromal epigenetic alterations drive metabolic and neuroendocrine prostate cancer reprogramming. J. Clin. Invest. 128, 4472–4484. doi: 10.1172/jci99397

PubMed Abstract | CrossRef Full Text | Google Scholar

Mohamed, E., Sierra, R. A., Trillo-Tinoco, J., Cao, Y., Innamarato, P., Payne, K. K., et al. (2020). The Unfolded protein response mediator PERK governs myeloid cell-driven immunosuppression in tumors through inhibition of STING signaling. Immunity 52, 668.e7–682.e7. doi: 10.1016/j.immuni.2020.03.004

PubMed Abstract | CrossRef Full Text | Google Scholar

Montenegro, F., and Indraccolo, S. (2020). Metabolism in the tumor microenvironment. Adv. Exp. Med. Biol. 1263, 1–11. doi: 10.1007/978-3-030-44518-8_1

CrossRef Full Text | Google Scholar

Moradi-Chaleshtori, M., Bandehpour, M., Soudi, S., Mohammadi-Yeganeh, S., and Hashemi, S. M. (2020). In vitro and in vivo evaluation of anti-tumoral effect of M1 phenotype induction in macrophages by miR-130 and miR-33 containing exosomes. Cancer Immunol. Immunother. 70, 1323–1339. doi: 10.1007/s00262-020-02762-x

PubMed Abstract | CrossRef Full Text | Google Scholar

Mudry, R. E., Fortney, J. E., York, T., Hall, B. M., and Gibson, L. F. (2000). Stromal cells regulate survival of B-lineage leukemic cells during chemotherapy. Blood 96, 1926–1932.

Google Scholar

Mukherjee, A., Chiang, C. Y., Daifotis, H. A., Nieman, K. M., Fahrmann, J. F., Lastra, R. R., et al. (2020). Adipocyte-induced FABP4 expression in ovarian cancer cells promotes metastasis and mediates carboplatin resistance. Cancer Res. 80, 1748–1761. doi: 10.1158/0008-5472.Can-19-1999

PubMed Abstract | CrossRef Full Text | Google Scholar

Muller, C. (2013). Tumour-surrounding adipocytes are active players in breast cancer progression. Ann. Endocrinol. 74, 108–110. doi: 10.1016/j.ando.2013.02.007

PubMed Abstract | CrossRef Full Text | Google Scholar

Muñoz-Garcia, J., Cochonneau, D., Télétchéa, S., Moranton, E., Lanoe, D., Brion, R., et al. (2021). The twin cytokines interleukin-34 and CSF-1: masterful conductors of macrophage homeostasis. Theranostics 11, 1568–1593. doi: 10.7150/thno.50683

PubMed Abstract | CrossRef Full Text | Google Scholar

Nagl, L., Horvath, L., Pircher, A., and Wolf, D. (2020). Tumor endothelial cells (TECs) as potential immune directors of the tumor microenvironment – new findings and future perspectives. Front. Cell Dev. Biol. 8:766. doi: 10.3389/fcell.2020.00766

PubMed Abstract | CrossRef Full Text | Google Scholar

Naito, H., Wakabayashi, T., Kidoya, H., Muramatsu, F., Takara, K., Eino, D., et al. (2016). Endothelial side population cells contribute to tumor angiogenesis and antiangiogenic drug resistance. Cancer Res. 76, 3200–3210. doi: 10.1158/0008-5472.Can-15-2998

PubMed Abstract | CrossRef Full Text | Google Scholar

Najafi, M., Goradel, N. H., Farhood, B., Salehi, E., Solhjoo, S., Toolee, H., et al. (2019). Tumor microenvironment: Interactions and therapy. J. Cell Physiol. 234, 5700–5721. doi: 10.1002/jcp.27425

PubMed Abstract | CrossRef Full Text | Google Scholar

Nieman, K. M., Kenny, H. A., Penicka, C. V., Ladanyi, A., Buell-Gutbrod, R., Zillhardt, M. R., et al. (2011). Adipocytes promote ovarian cancer metastasis and provide energy for rapid tumor growth. Nat. Med. 17, 1498–1503. doi: 10.1038/nm.2492

PubMed Abstract | CrossRef Full Text | Google Scholar

Nieman, K. M., Romero, I. L., Van Houten, B., and Lengyel, E. (2013). Adipose tissue and adipocytes support tumorigenesis and metastasis. Biochim. Biophys. Acta Mol. Cell Biol. Lipids 1831, 1533–1541. doi: 10.1016/j.bbalip.2013.02.010

PubMed Abstract | CrossRef Full Text | Google Scholar

Nilsson, M. B., Sun, H., Robichaux, J., Pfeifer, M., McDermott, U., Travers, J., et al. (2020). A YAP/FOXM1 axis mediates EMT-associated EGFR inhibitor resistance and increased expression of spindle assembly checkpoint components. Sci. Transl. Med. 12:eaaz4589. doi: 10.1126/scitranslmed.aaz4589

PubMed Abstract | CrossRef Full Text | Google Scholar

Nywening, T. M., Belt, B. A., Cullinan, D. R., Panni, R. Z., Han, B. J., Sanford, D. E., et al. (2018). Targeting both tumour-associated CXCR2(+) neutrophils and CCR2(+) macrophages disrupts myeloid recruitment and improves chemotherapeutic responses in pancreatic ductal adenocarcinoma. Gut 67, 1112–1123. doi: 10.1136/gutjnl-2017-313738

PubMed Abstract | CrossRef Full Text | Google Scholar

Oevermann, L., Scheitz, J., Starke, K., Köck, K., Kiefer, T., Dölken, G., et al. (2009). Hematopoietic stem cell differentiation affects expression and function of MRP4 (ABCC4), a transport protein for signaling molecules and drugs. Int. J. Cancer 124, 2303–2311. doi: 10.1002/ijc.24207

PubMed Abstract | CrossRef Full Text | Google Scholar

Orimo, A., and Weinberg, R. A. (2006). Stromal fibroblasts in cancer: a novel tumor-promoting cell type. Cell Cycle 5, 1597–1601. doi: 10.4161/cc.5.15.3112

PubMed Abstract | CrossRef Full Text | Google Scholar

Oweida, A., Hararah, M. K., Phan, A., Binder, D., Bhatia, S., Lennon, S., et al. (2018). Resistance to radiotherapy and PD-L1 blockade is mediated by TIM-3 upregulation and regulatory t-cell infiltration. Clin. Cancer Res. 24, 5368–5380. doi: 10.1158/1078-0432.CCR-18-1038

PubMed Abstract | CrossRef Full Text | Google Scholar

Özdemir, B. C., Pentcheva-Hoang, T., Carstens, J. L., Zheng, X., Wu, C.-C., Simpson, T. R., et al. (2015). Depletion of carcinoma-associated fibroblasts and fibrosis induces immunosuppression and accelerates pancreas cancer with reduced survival. Cancer Cell 28, 831–833. doi: 10.1016/j.ccell.2015.11.002

PubMed Abstract | CrossRef Full Text | Google Scholar

Paget, S. (1989). The distribution of secondary growths in cancer of the breast. 1889. Cancer Metastasis Rev. 8, 98–101.

Google Scholar

Park, J., Morley, T. S., and Scherer, P. E. (2013). Inhibition of endotrophin, a cleavage product of collagen VI, confers cisplatin sensitivity to tumours. EMBO Mol. Med. 5, 935–948. doi: 10.1002/emmm.201202006

PubMed Abstract | CrossRef Full Text | Google Scholar

Pascual, G., Avgustinova, A., Mejetta, S., Martín, M., Castellanos, A., Attolini, C. S., et al. (2017). Targeting metastasis-initiating cells through the fatty acid receptor CD36. Nature 541, 41–45. doi: 10.1038/nature20791

PubMed Abstract | CrossRef Full Text | Google Scholar

Patocs, A., Zhang, L., Xu, Y., Weber, F., Caldes, T., Mutter, G. L., et al. (2007). Breast-cancer stromal cells with TP53 mutations and nodal metastases. N. Engl. J. Med. 357, 2543–2551. doi: 10.1056/NEJMoa071825

PubMed Abstract | CrossRef Full Text | Google Scholar

Paunescu, V., Bojin, F. M., Tatu, C. A., Gavriliuc, O. I., Rosca, A., Gruia, A. T., et al. (2011). Tumour-associated fibroblasts and mesenchymal stem cells: more similarities than differences. J. Cell Mol. Med. 15, 635–646. doi: 10.1111/j.1582-4934.2010.01044.x

PubMed Abstract | CrossRef Full Text | Google Scholar

Pérez de Heredia, F., Wood, I. S., and Trayhurn, P. (2010). Hypoxia stimulates lactate release and modulates monocarboxylate transporter (MCT1, MCT2, and MCT4) expression in human adipocytes. Pflugers Arch. 459, 509–518. doi: 10.1007/s00424-009-0750-3

PubMed Abstract | CrossRef Full Text | Google Scholar

Perrotta, C., Cervia, D., Di Renzo, I., Moscheni, C., Bassi, M. T., Campana, L., et al. (2018). Nitric Oxide generated by tumor-associated macrophages is responsible for cancer resistance to cisplatin and correlated with syntaxin 4 and acid sphingomyelinase inhibition. Front. Immunol. 9:1186. doi: 10.3389/fimmu.2018.01186

PubMed Abstract | CrossRef Full Text | Google Scholar

Pértega-Gomes, N., Vizcaíno, J. R., Attig, J., Jurmeister, S., Lopes, C., and Baltazar, F. (2014). A lactate shuttle system between tumour and stromal cells is associated with poor prognosis in prostate cancer. BMC Cancer 14:352. doi: 10.1186/1471-2407-14-352

PubMed Abstract | CrossRef Full Text | Google Scholar

Pertusini, E., Ratajczak, J., Majka, M., Vaughn, D., Ratajczak, M. Z., and Gewirtz, A. M. (2001). Investigating the platelet-sparing mechanism of paclitaxel/carboplatin combination chemotherapy. Blood 97, 638–644. doi: 10.1182/blood.v97.3.638

PubMed Abstract | CrossRef Full Text | Google Scholar

Pistore, C., Giannoni, E., Colangelo, T., Rizzo, F., Magnani, E., Muccillo, L., et al. (2017). DNA methylation variations are required for epithelial-to-mesenchymal transition induced by cancer-associated fibroblasts in prostate cancer cells. Oncogene 36, 5551–5566. doi: 10.1038/onc.2017.159

PubMed Abstract | CrossRef Full Text | Google Scholar

Pramanik, R., Sheng, X., Ichihara, B., Heisterkamp, N., and Mittelman, S. D. (2013). Adipose tissue attracts and protects acute lymphoblastic leukemia cells from chemotherapy. Leuk. Res. 37, 503–509. doi: 10.1016/j.leukres.2012.12.013

PubMed Abstract | CrossRef Full Text | Google Scholar

Pylaeva, E., Lang, S., and Jablonska, J. (2016). The essential role of Type I interferons in differentiation and activation of tumor-associated neutrophils. Front. Immunol. 7:629. doi: 10.3389/fimmu.2016.00629

PubMed Abstract | CrossRef Full Text | Google Scholar

Qiao, Y., Zhang, C., Li, A., Wang, D., Luo, Z., Ping, Y., et al. (2018). IL6 derived from cancer-associated fibroblasts promotes chemoresistance via CXCR7 in esophageal squamous cell carcinoma. Oncogene 37, 873–883. doi: 10.1038/onc.2017.387

PubMed Abstract | CrossRef Full Text | Google Scholar

Qin, X., Guo, H., Wang, X., Zhu, X., Yan, M., Wang, X., et al. (2019). Exosomal miR-196a derived from cancer-associated fibroblasts confers cisplatin resistance in head and neck cancer through targeting CDKN1B and ING5. Genome Biol. 20:12. doi: 10.1186/s13059-018-1604-0

PubMed Abstract | CrossRef Full Text | Google Scholar

Rachidi, S., Metelli, A., Riesenberg, B., Wu, B. X., Nelson, M. H., Wallace, C., et al. (2017). Platelets subvert T cell immunity against cancer via GARP-TGFβ axis. Sci. Immunol. 2:eaai7911. doi: 10.1126/sciimmunol.aai7911

PubMed Abstract | CrossRef Full Text | Google Scholar

Radziwon-Balicka, A., Medina, C., O’Driscoll, L., Treumann, A., Bazou, D., Inkielewicz-Stepniak, I., et al. (2012). Platelets increase survival of adenocarcinoma cells challenged with anticancer drugs: mechanisms and implications for chemoresistance. Br. J. Pharmacol. 167, 787–804. doi: 10.1111/j.1476-5381.2012.01991.x

PubMed Abstract | CrossRef Full Text | Google Scholar

Raghavan, S., Snyder, C. S., Wang, A., McLean, K., Zamarin, D., Buckanovich, R. J., et al. (2020). Carcinoma-associated mesenchymal stem cells promote chemoresistance in ovarian cancer stem Cells via PDGF signaling. Cancers 12:2063. doi: 10.3390/cancers12082063

PubMed Abstract | CrossRef Full Text | Google Scholar

Ramesh, A., Kumar, S., Nandi, D., and Kulkarni, A. (2019). CSF1R- and SHP2-inhibitor-loaded nanoparticles enhance cytotoxic activity and phagocytosis in tumor-associated macrophages. Adv. Mater. 31:e1904364. doi: 10.1002/adma.201904364

PubMed Abstract | CrossRef Full Text | Google Scholar

Reagan, M. R., and Kaplan, D. L. (2011). Concise review: mesenchymal stem cell tumor-homing: detection methods in disease model systems. Stem Cells 29, 920–927. doi: 10.1002/stem.645

PubMed Abstract | CrossRef Full Text | Google Scholar

Ren, J., Ding, L., Zhang, D., Shi, G., Xu, Q., Shen, S., et al. (2018). Carcinoma-associated fibroblasts promote the stemness and chemoresistance of colorectal cancer by transferring exosomal lncRNA H19. Theranostics 8, 3932–3948. doi: 10.7150/thno.25541

PubMed Abstract | CrossRef Full Text | Google Scholar

Richards, K. E., Zeleniak, A. E., Fishel, M. L., Wu, J., Littlepage, L. E., and Hill, R. (2017). Cancer-associated fibroblast exosomes regulate survival and proliferation of pancreatic cancer cells. Oncogene 36, 1770–1778. doi: 10.1038/onc.2016.353

PubMed Abstract | CrossRef Full Text | Google Scholar

Rodriguez-Canales, J., Hanson, J. C., Tangrea, M. A., Erickson, H. S., Albert, P. S., Wallis, B. S., et al. (2007). Identification of a unique epigenetic sub-microenvironment in prostate cancer. J. Pathol. 211, 410–419. doi: 10.1002/path.2133

PubMed Abstract | CrossRef Full Text | Google Scholar

Romano, A., Parrinello, N. L., La Cava, P., Tibullo, D., Giallongo, C., Camiolo, G., et al. (2018). PMN-MDSC and arginase are increased in myeloma and may contribute to resistance to therapy. Expert Rev. Mol. Diagn. 18, 675–683. doi: 10.1080/14737159.2018.1470929

PubMed Abstract | CrossRef Full Text | Google Scholar

Rong, Y., Yuan, C. H., Qu, Z., Zhou, H., Guan, Q., Yang, N., et al. (2016). Doxorubicin resistant cancer cells activate myeloid-derived suppressor cells by releasing PGE2. Sci. Rep. 6:23824. doi: 10.1038/srep23824

PubMed Abstract | CrossRef Full Text | Google Scholar

Roodhart, J. M., Daenen, L. G., Stigter, E. C., Prins, H. J., Gerrits, J., Houthuijzen, J. M., et al. (2011). Mesenchymal stem cells induce resistance to chemotherapy through the release of platinum-induced fatty acids. Cancer Cell 20, 370–383. doi: 10.1016/j.ccr.2011.08.010

PubMed Abstract | CrossRef Full Text | Google Scholar

Sansone, P., Savini, C., Kurelac, I., Chang, Q., Amato, L. B., Strillacci, A., et al. (2017). Packaging and transfer of mitochondrial DNA via exosomes regulate escape from dormancy in hormonal therapy-resistant breast cancer. Proc. Natl. Acad. Sci. U.S.A. 114, E9066–E9075. doi: 10.1073/pnas.1704862114

PubMed Abstract | CrossRef Full Text | Google Scholar

Sapudom, J., Müller, C. D., Nguyen, K. T., Martin, S., Anderegg, U., and Pompe, T. (2020). Matrix remodeling and hyaluronan production by myofibroblasts and cancer-associated fibroblasts in 3D collagen matrices. Gels 6:33. doi: 10.3390/gels6040033

PubMed Abstract | CrossRef Full Text | Google Scholar

Satoh, M., Cherian, M. G., Imura, N., and Shimizu, H. (1994). Modulation of resistance to anticancer drugs by inhibition of metallothionein synthesis. Cancer Res. 54, 5255–5257.

Google Scholar

Schaaf, M. B., Garg, A. D., and Agostinis, P. (2018). Defining the role of the tumor vasculature in antitumor immunity and immunotherapy. Cell Death Dis. 9:115. doi: 10.1038/s41419-017-0061-0

PubMed Abstract | CrossRef Full Text | Google Scholar

Scherzed, A., Hackenberg, S., Froelich, K., Kessler, M., Koehler, C., Hagen, R., et al. (2011). BMSC enhance the survival of paclitaxel treated squamous cell carcinoma cells in vitro. Cancer Biol. Ther. 11, 349–357. doi: 10.4161/cbt.11.3.14179

PubMed Abstract | CrossRef Full Text | Google Scholar

Schlenk, R. F., Paschka, P., Krzykalla, J., Weber, D., Kapp-Schwoerer, S., Gaidzik, V. I., et al. (2020). Gemtuzumab ozogamicin in – mutated acute myeloid leukemia: early results from the prospective randomized AMLSG 09-09 Phase III study. J. Clin. Oncol. 38, 623–632. doi: 10.1200/JCO.19.01406

PubMed Abstract | CrossRef Full Text | Google Scholar

Schuler, P. J., Harasymczuk, M., Schilling, B., Saze, Z., Strauss, L., Lang, S., et al. (2013). Effects of adjuvant chemoradiotherapy on the frequency and function of regulatory T cells in patients with head and neck cancer. Clin. Cancer Res. 19, 6585–6596. doi: 10.1158/1078-0432.Ccr-13-0900

PubMed Abstract | CrossRef Full Text | Google Scholar

Senthebane, D. A., Rowe, A., Thomford, N. E., Shipanga, H., Munro, D., Mazeedi, M., et al. (2017). The role of tumor microenvironment in chemoresistance: to survive, keep your enemies closer. Int. J. Mol. Sci. 18:1586. doi: 10.3390/ijms18071586

PubMed Abstract | CrossRef Full Text | Google Scholar

Shah, K., and Rawal, R. M. (2019). Genetic and epigenetic modulation of drug resistance in cancer: challenges and opportunities. Curr. Drug Metab. 20, 1114–1131. doi: 10.2174/1389200221666200103111539

PubMed Abstract | CrossRef Full Text | Google Scholar

Shan, L. (2004). “FluidMAG iron nanoparticle-labeled mesenchymal stem cells for tracking cell homing to tumors,” in Molecular Imaging and Contrast Agent Database (MICAD), (Bethesda, MD: National Center for Biotechnology Information (US).).

Google Scholar

Sheng, X., Parmentier, J. H., Tucci, J., Pei, H., Cortez-Toledo, O., Dieli-Conwright, C. M., et al. (2017). Adipocytes sequester and metabolize the chemotherapeutic daunorubicin. Mol. Cancer Res. 15, 1704–1713. doi: 10.1158/1541-7786.MCR-17-0338

PubMed Abstract | CrossRef Full Text | Google Scholar

Sherman-Baust, C. A., Weeraratna, A. T., Rangel, L. B., Pizer, E. S., Cho, K. R., Schwartz, D. R., et al. (2003). Remodeling of the extracellular matrix through overexpression of collagen VI contributes to cisplatin resistance in ovarian cancer cells. Cancer Cell 3, 377–386. doi: 10.1016/s1535-6108(03)00058-8

CrossRef Full Text | Google Scholar

Shi, Y., Du, L., Lin, L., and Wang, Y. (2017). Tumour-associated mesenchymal stem/stromal cells: emerging therapeutic targets. Nat. Rev. Drug Discov. 16, 35–52. doi: 10.1038/nrd.2016.193

PubMed Abstract | CrossRef Full Text | Google Scholar

Shibue, T., and Weinberg, R. A. (2017). EMT, CSCs, and drug resistance: the mechanistic link and clinical implications. Nat. Rev. Clin. Oncol. 14, 611–629. doi: 10.1038/nrclinonc.2017.44

PubMed Abstract | CrossRef Full Text | Google Scholar

Shien, K., Papadimitrakopoulou, V. A., Ruder, D., Behrens, C., Shen, L., Kalhor, N., et al. (2017). JAK1/STAT3 activation through a proinflammatory cytokine pathway leads to resistance to molecularly targeted therapy in non-small cell lung cancer. Mol. Cancer Ther. 16, 2234–2245. doi: 10.1158/1535-7163.Mct-17-0148

PubMed Abstract | CrossRef Full Text | Google Scholar

Shree, T., Olson, O. C., Elie, B. T., Kester, J. C., Garfall, A. L., Simpson, K., et al. (2011). Macrophages and cathepsin proteases blunt chemotherapeutic response in breast cancer. Genes Dev. 25, 2465–2479. doi: 10.1101/gad.180331.111

PubMed Abstract | CrossRef Full Text | Google Scholar

Siegel, R. L., Miller, K. D., and Jemal, A. (2020). Cancer statistics, 2020. CA Cancer J. Clin. 70, 7–30. doi: 10.3322/caac.21590

PubMed Abstract | CrossRef Full Text | Google Scholar

Siska, P. J., Singer, K., Evert, K., Renner, K., and Kreutz, M. (2020). The immunological Warburg effect: can a metabolic-tumor-stroma score (MeTS) guide cancer immunotherapy? Immunol. Rev. 295, 187–202. doi: 10.1111/imr.12846

PubMed Abstract | CrossRef Full Text | Google Scholar

Soda, Y., Marumoto, T., Friedmann-Morvinski, D., Soda, M., Liu, F., Michiue, H., et al. (2011). Transdifferentiation of glioblastoma cells into vascular endothelial cells. Proc. Natil. Acad. Sci. U.S.A. 108, 4274–4280. doi: 10.1073/pnas.1016030108

PubMed Abstract | CrossRef Full Text | Google Scholar

Stapor, P., Wang, X., Goveia, J., Moens, S., and Carmeliet, P. (2014). Angiogenesis revisited – role and therapeutic potential of targeting endothelial metabolism. J. Cell Sci. 127(Pt 20), 4331–4341. doi: 10.1242/jcs.153908

PubMed Abstract | CrossRef Full Text | Google Scholar

Steinberg, S. M., Shabaneh, T. B., Zhang, P., Martyanov, V., Li, Z., Malik, B. T., et al. (2017). Myeloid cells that impair immunotherapy are restored in melanomas with acquired resistance to BRAF Inhibitors. Cancer Res. 77, 1599–1610. doi: 10.1158/0008-5472.Can-16-1755

PubMed Abstract | CrossRef Full Text | Google Scholar

Sugimoto, H., Mundel, T. M., Kieran, M. W., and Kalluri, R. (2006). Identification of fibroblast heterogeneity in the tumor microenvironment. Cancer Biol. Ther. 5, 1640–1646. doi: 10.4161/cbt.5.12.3354

PubMed Abstract | CrossRef Full Text | Google Scholar

Sugimura, K., Miyata, H., Tanaka, K., Takahashi, T., Kurokawa, Y., Yamasaki, M., et al. (2015). High infiltration of tumor-associated macrophages is associated with a poor response to chemotherapy and poor prognosis of patients undergoing neoadjuvant chemotherapy for esophageal cancer. J. Surg. Oncol. 111, 752–759. doi: 10.1002/jso.23881

PubMed Abstract | CrossRef Full Text | Google Scholar

Suzuki, E., Yamazaki, S., Naito, T., Hashimoto, H., Okubo, S., Udagawa, H., et al. (2019). Secretion of high amounts of hepatocyte growth factor is a characteristic feature of cancer-associated fibroblasts with EGFR-TKI resistance-promoting phenotype: a study of 18 cases of cancer-associated fibroblasts. Pathol. Int. 69, 472–480. doi: 10.1111/pin.12838

PubMed Abstract | CrossRef Full Text | Google Scholar

Talmadge, J. E., and Gabrilovich, D. I. (2013). History of myeloid-derived suppressor cells. Nat. Rev. Cancer 13, 739–752. doi: 10.1038/nrc3581

PubMed Abstract | CrossRef Full Text | Google Scholar

Tanaka, K., Miyata, H., Sugimura, K., Fukuda, S., Kanemura, T., Yamashita, K., et al. (2015). miR-27 is associated with chemoresistance in esophageal cancer through transformation of normal fibroblasts to cancer-associated fibroblasts. Carcinogenesis 36, 894–903. doi: 10.1093/carcin/bgv067

PubMed Abstract | CrossRef Full Text | Google Scholar

Tang, Y. A., Chen, Y. F., Bao, Y., Mahara, S., Yatim, S., Oguz, G., et al. (2018). Hypoxic tumor microenvironment activates GLI2 via HIF-1α and TGF-β2 to promote chemoresistance in colorectal cancer. Proc. Natl. Acad. Sci. U.S.A. 115, E5990–E5999. doi: 10.1073/pnas.1801348115

PubMed Abstract | CrossRef Full Text | Google Scholar

Tao, L., Huang, G., Wang, R., Pan, Y., He, Z., Chu, X., et al. (2016). Cancer-associated fibroblasts treated with cisplatin facilitates chemoresistance of lung adenocarcinoma through IL-11/IL-11R/STAT3 signaling pathway. Sci. Rep. 6:38408. doi: 10.1038/srep38408

PubMed Abstract | CrossRef Full Text | Google Scholar

Tavora, B., Reynolds, L. E., Batista, S., Demircioglu, F., Fernandez, I., Lechertier, T., et al. (2014). Endothelial-cell FAK targeting sensitizes tumours to DNA-damaging therapy. Nature 514, 112–116. doi: 10.1038/nature13541

PubMed Abstract | CrossRef Full Text | Google Scholar

Teng, F., Tian, W. Y., Wang, Y. M., Zhang, Y. F., Guo, F., Zhao, J., et al. (2016). Cancer-associated fibroblasts promote the progression of endometrial cancer via the SDF-1/CXCR4 axis. J. Hematol. Oncol. 9:8. doi: 10.1186/s13045-015-0231-4

PubMed Abstract | CrossRef Full Text | Google Scholar

Teng, I. W., Hou, P. C., Lee, K. D., Chu, P. Y., Yeh, K. T., Jin, V. X., et al. (2011). Targeted methylation of two tumor suppressor genes is sufficient to transform mesenchymal stem cells into cancer stem/initiating cells. Cancer Res. 71, 4653–4663. doi: 10.1158/0008-5472.CAN-10-3418

PubMed Abstract | CrossRef Full Text | Google Scholar

Tesfamariam, B. (2016). Involvement of platelets in tumor cell metastasis. Pharmacol. Ther. 157, 112–119. doi: 10.1016/j.pharmthera.2015.11.005

PubMed Abstract | CrossRef Full Text | Google Scholar

Tu, B., Zhu, J., Liu, S., Wang, L., Fan, Q., Hao, Y., et al. (2016). Mesenchymal stem cells promote osteosarcoma cell survival and drug resistance through activation of STAT3. Oncotarget 7, 48296–48308. doi: 10.18632/oncotarget.10219

PubMed Abstract | CrossRef Full Text | Google Scholar

Vaidya, F. U., Sufiyan Chhipa, A., Mishra, V., Gupta, V. K., Rawat, S. G., Kumar, A., et al. (2020). Molecular and cellular paradigms of multidrug resistance in cancer. Cancer Rep. e1291. doi: 10.1002/cnr2.1291 [Epub ahead of print].

CrossRef Full Text | PubMed Abstract | Google Scholar

van Beijnum, J. R., Nowak-Sliwinska, P., Huijbers, E. J., Thijssen, V. L., and Griffioen, A. W. (2015). The great escape; the hallmarks of resistance to antiangiogenic therapy. Pharmacol. Rev. 67, 441–461. doi: 10.1124/pr.114.010215

PubMed Abstract | CrossRef Full Text | Google Scholar

Van Damme, H., Dombrecht, B., Kiss, M., Roose, H., Allen, E., Van Overmeire, E., et al. (2021). Therapeutic depletion of CCR8 tumor-infiltrating regulatory T cells elicits antitumor immunity and synergizes with anti-PD-1 therapy. J. Immunother. Cancer 9:e001749. doi: 10.1136/jitc-2020-001749

PubMed Abstract | CrossRef Full Text | Google Scholar

Vennin, C., Mélénec, P., Rouet, R., Nobis, M., Cazet, A. S., Murphy, K. J., et al. (2019). CAF hierarchy driven by pancreatic cancer cell p53-status creates a pro-metastatic and chemoresistant environment via perlecan. Nat. Commun. 10:3637. doi: 10.1038/s41467-019-10968-6

PubMed Abstract | CrossRef Full Text | Google Scholar

Vianello, F., Villanova, F., Tisato, V., Lymperi, S., Ho, K. K., Gomes, A. R., et al. (2010). Bone marrow mesenchymal stromal cells non-selectively protect chronic myeloid leukemia cells from imatinib-induced apoptosis via the CXCR4/CXCL12 axis. Haematologica 95, 1081–1089. doi: 10.3324/haematol.2009.017178

PubMed Abstract | CrossRef Full Text | Google Scholar

von Einem, J. C., Guenther, C., Volk, H. D., Grütz, G., Hirsch, D., Salat, C., et al. (2019). Treatment of advanced gastrointestinal cancer with genetically modified autologous mesenchymal stem cells: results from the phase 1/2 TREAT-ME-1 trial. Int. J. Cancer 145, 1538–1546. doi: 10.1002/ijc.32230

PubMed Abstract | CrossRef Full Text | Google Scholar

Wang, D., Yang, L., Yu, W., Wu, Q., Lian, J., Li, F., et al. (2019). Colorectal cancer cell-derived CCL20 recruits regulatory T cells to promote chemoresistance via FOXO1/CEBPB/NF-κB signaling. J. Immunother. Cancer 7:215. doi: 10.1186/s40425-019-0701-2

PubMed Abstract | CrossRef Full Text | Google Scholar

Wang, J., Cui, R., Clement, C. G., Nawgiri, R., Powell, D. W., Pinchuk, I. V., et al. (2020). Activation PDGFR-α/AKT mediated signaling pathways in oral squamous cell carcinoma by mesenchymal stem/stromal cells promotes anti-apoptosis and decreased sensitivity to cisplatin. Front. Oncol. 10:552. doi: 10.3389/fonc.2020.00552

PubMed Abstract | CrossRef Full Text | Google Scholar

Wang, J., Hendrix, A., Hernot, S., Lemaire, M., De Bruyne, E., Van Valckenborgh, E., et al. (2014). Bone marrow stromal cell-derived exosomes as communicators in drug resistance in multiple myeloma cells. Blood 124, 555–566. doi: 10.1182/blood-2014-03-562439

PubMed Abstract | CrossRef Full Text | Google Scholar

Wang, J., Liu, X., Qiu, Y., Shi, Y., Cai, J., Wang, B., et al. (2018). Cell adhesion-mediated mitochondria transfer contributes to mesenchymal stem cell-induced chemoresistance on T cell acute lymphoblastic leukemia cells. J. Hematol. Oncol. 11:11. doi: 10.1186/s13045-018-0554-z

PubMed Abstract | CrossRef Full Text | Google Scholar

Wang, L., Li, X., Ren, Y., Geng, H., Zhang, Q., Cao, L., et al. (2019). Cancer-associated fibroblasts contribute to cisplatin resistance by modulating ANXA3 in lung cancer cells. Cancer Sci. 110, 1609–1620. doi: 10.1111/cas.13998

PubMed Abstract | CrossRef Full Text | Google Scholar

Wang, S., Wang, X., Liu, S., Zhang, S., Wei, X., Song, Y., et al. (2020). The CXCR4 antagonist, AMD3100, reverses mesenchymal stem cell-mediated drug resistance in relapsed/refractory acute lymphoblastic leukemia. OncoTargets Ther. 13, 6583–6591. doi: 10.2147/ott.S249425

PubMed Abstract | CrossRef Full Text | Google Scholar

Wang, Z., Fang, M., Li, J., Yang, R., Du, J., and Luo, Y. (2018). High platelet levels attenuate the efficacy of platinum-based treatment in non-small cell lung cancer. Cell. Physiol. Biochem. 48, 2456–2469. doi: 10.1159/000492683

PubMed Abstract | CrossRef Full Text | Google Scholar

Wei, L., Ye, H., Li, G., Lu, Y., Zhou, Q., Zheng, S., et al. (2018). Cancer-associated fibroblasts promote progression and gemcitabine resistance via the SDF-1/SATB-1 pathway in pancreatic cancer. Cell Death Dis. 9:1065. doi: 10.1038/s41419-018-1104-x

PubMed Abstract | CrossRef Full Text | Google Scholar

Weizman, N., Krelin, Y., Shabtay-Orbach, A., Amit, M., Binenbaum, Y., Wong, R. J., et al. (2014). Macrophages mediate gemcitabine resistance of pancreatic adenocarcinoma by upregulating cytidine deaminase. Oncogene 33, 3812–3819. doi: 10.1038/onc.2013.357

PubMed Abstract | CrossRef Full Text | Google Scholar

Wen, X., He, X., Jiao, F., Wang, C., Sun, Y., Ren, X., et al. (2017). Fibroblast activation protein-α-positive fibroblasts promote gastric cancer progression and resistance to immune checkpoint blockade. Oncol. Res. 25, 629–640. doi: 10.3727/096504016x14768383625385

PubMed Abstract | CrossRef Full Text | Google Scholar

Wu, H., Liu, B., Chen, Z., Li, G., and Zhang, Z. (2020). MSC-induced lncRNA HCP5 drove fatty acid oxidation through miR-3619-5p/AMPK/PGC1alpha/CEBPB axis to promote stemness and chemo-resistance of gastric cancer. Cell Death Dis. 11:233. doi: 10.1038/s41419-020-2426-z

PubMed Abstract | CrossRef Full Text | Google Scholar

Wu, Q., Zhou, W., Yin, S., Zhou, Y., Chen, T., Qian, J., et al. (2019). Blocking triggering receptor expressed on myeloid cells-1-positive tumor-associated macrophages induced by hypoxia reverses immunosuppression and anti-programmed cell death ligand 1 resistance in liver cancer. Hepatology 70, 198–214. doi: 10.1002/hep.30593

PubMed Abstract | CrossRef Full Text | Google Scholar

Xiong, Y. Q., Sun, H. C., Zhang, W., Zhu, X. D., Zhuang, P. Y., Zhang, J. B., et al. (2009). Human hepatocellular carcinoma tumor-derived endothelial cells manifest increased angiogenesis capability and drug resistance compared with normal endothelial cells. Clin. Cancer Res. 15, 4838–4846. doi: 10.1158/1078-0432.CCR-08-2780

PubMed Abstract | CrossRef Full Text | Google Scholar

Xu, H., Zhou, Y., Li, W., Zhang, B., Zhang, H., Zhao, S., et al. (2018). Tumor-derived mesenchymal-stem-cell-secreted IL-6 enhances resistance to cisplatin via the STAT3 pathway in breast cancer. Oncol. Lett. 15, 9142–9150. doi: 10.3892/ol.2018.8463

PubMed Abstract | CrossRef Full Text | Google Scholar

Xu, M., Zhao, Z., Song, J., Lan, X., Lu, S., Chen, M., et al. (2017). Interactions between interleukin-6 and myeloid-derived suppressor cells drive the chemoresistant phenotype of hepatocellular cancer. Exp. Cell Res. 351, 142–149. doi: 10.1016/j.yexcr.2017.01.008

PubMed Abstract | CrossRef Full Text | Google Scholar

Xu, S. S., Xu, H. X., Wang, W. Q., Li, S., Li, H., Li, T. J., et al. (2019). Tumor-infiltrating platelets predict postoperative recurrence and survival in resectable pancreatic neuroendocrine tumor. World J. Gastroenterol. 25, 6248–6257. doi: 10.3748/wjg.v25.i41.6248

PubMed Abstract | CrossRef Full Text | Google Scholar

Xu, X., Ye, J., Huang, C., Yan, Y., and Li, J. (2019). M2 macrophage-derived IL6 mediates resistance of breast cancer cells to hedgehog inhibition. Toxicol. Appl. Pharmacol. 364, 77–82. doi: 10.1016/j.taap.2018.12.013

PubMed Abstract | CrossRef Full Text | Google Scholar

Yamaguchi, R., and Perkins, G. (2018). Animal models for studying tumor microenvironment (TME) and resistance to lymphocytic infiltration. Cancer Biol. Ther. 19, 745–754. doi: 10.1080/15384047.2018.1470722

PubMed Abstract | CrossRef Full Text | Google Scholar

Yan, H., Guo, B. Y., and Zhang, S. (2016). Cancer-associated fibroblasts attenuate Cisplatin-induced apoptosis in ovarian cancer cells by promoting STAT3 signaling. Biochem. Biophys. Res. Commun. 470, 947–954. doi: 10.1016/j.bbrc.2016.01.131

PubMed Abstract | CrossRef Full Text | Google Scholar

Yang, C., He, L., He, P., Liu, Y., Wang, W., He, Y., et al. (2015). Increased drug resistance in breast cancer by tumor-associated macrophages through IL-10/STAT3/bcl-2 signaling pathway. Med. Oncol. 32:352. doi: 10.1007/s12032-014-0352-6

PubMed Abstract | CrossRef Full Text | Google Scholar

Yang, E., Wang, X., Gong, Z., Yu, M., Wu, H., and Zhang, D. (2020). Exosome-mediated metabolic reprogramming: the emerging role in tumor microenvironment remodeling and its influence on cancer progression. Signal. Transduct. Target Ther. 5:242. doi: 10.1038/s41392-020-00359-5

PubMed Abstract | CrossRef Full Text | Google Scholar

Yang, J., Zaman, M. M., Vlasakov, I., Roy, R., Huang, L., Martin, C. R., et al. (2019). Adipocytes promote ovarian cancer chemoresistance. Sci. Rep. 9:13316. doi: 10.1038/s41598-019-49649-1

PubMed Abstract | CrossRef Full Text | Google Scholar

Yeung, C. L. A., Co, N.-N., Tsuruga, T., Yeung, T.-L., Kwan, S.-Y., Leung, C. S., et al. (2016). Exosomal transfer of stroma-derived miR21 confers paclitaxel resistance in ovarian cancer cells through targeting APAF1. Nat. Commun. 7:11150. doi: 10.1038/ncomms11150

PubMed Abstract | CrossRef Full Text | Google Scholar

Yi, Y., Zeng, S., Wang, Z., Wu, M., Ma, Y., Ye, X., et al. (2018). Cancer-associated fibroblasts promote epithelial-mesenchymal transition and EGFR-TKI resistance of non-small cell lung cancers via HGF/IGF-1/ANXA2 signaling. Biochim. Biophys. Acta Mol. Basis Dis. 1864, 793–803. doi: 10.1016/j.bbadis.2017.12.021

PubMed Abstract | CrossRef Full Text | Google Scholar

Yin, C., Evason, K. J., Asahina, K., and Stainier, D. Y. (2013). Hepatic stellate cells in liver development, regeneration, and cancer. J. Clin. Invest. 123, 1902–1910. doi: 10.1172/jci66369

PubMed Abstract | CrossRef Full Text | Google Scholar

Yin, X., Han, S., Song, C., Zou, H., Wei, Z., Xu, W., et al. (2019). Metformin enhances gefitinib efficacy by interfering with interactions between tumor-associated macrophages and head and neck squamous cell carcinoma cells. Cell Oncol. 42, 459–475. doi: 10.1007/s13402-019-00446-y

PubMed Abstract | CrossRef Full Text | Google Scholar

Yin, Y., Yao, S., Hu, Y., Feng, Y., Li, M., Bian, Z., et al. (2017). The immune-microenvironment confers chemoresistance of colorectal cancer through macrophage-derived IL6. Clin Cancer Res. 23, 7375–7387. doi: 10.1158/1078-0432.Ccr-17-1283

PubMed Abstract | CrossRef Full Text | Google Scholar

Yin, Z., Jiang, K., Li, R., Dong, C., and Wang, L. (2018). Multipotent mesenchymal stromal cells play critical roles in hepatocellular carcinoma initiation, progression and therapy. Mol. Cancer 17, 178. doi: 10.1186/s12943-018-0926-6

PubMed Abstract | CrossRef Full Text | Google Scholar

Yoshida, G. J. (2015). Metabolic reprogramming: the emerging concept and associated therapeutic strategies. J. Exp. Clin. Cancer Res. 34:111. doi: 10.1186/s13046-015-0221-y

PubMed Abstract | CrossRef Full Text | Google Scholar

You, J., Li, M., Cao, L. M., Gu, Q. H., Deng, P. B., Tan, Y., et al. (2019). Snail1-dependent cancer-associated fibroblasts induce epithelial-mesenchymal transition in lung cancer cells via exosomes. Qjm 112, 581–590. doi: 10.1093/qjmed/hcz093

PubMed Abstract | CrossRef Full Text | Google Scholar

Youn, J. I., Nagaraj, S., Collazo, M., and Gabrilovich, D. I. (2008). Subsets of myeloid-derived suppressor cells in tumor-bearing mice. J. Immunol. 181, 5791–5802. doi: 10.4049/jimmunol.181.8.5791

PubMed Abstract | CrossRef Full Text | Google Scholar

Yu, S., Li, Q., Yu, Y., Cui, Y., Li, W., Liu, T., et al. (2020). Activated HIF1α of tumor cells promotes chemoresistance development via recruiting GDF15-producing tumor-associated macrophages in gastric cancer. Cancer Immunol. Immunother. 69, 1973–1987. doi: 10.1007/s00262-020-02598-5

PubMed Abstract | CrossRef Full Text | Google Scholar

Yu, W., Cao, D.-D., Li, Q.-B., Mei, H.-L., Hu, Y., and Guo, T. (2016). Adipocytes secreted leptin is a pro-tumor factor for survival of multiple myeloma under chemotherapy. Oncotarget 7, 86075–86086. doi: 10.18632/oncotarget.13342

PubMed Abstract | CrossRef Full Text | Google Scholar

Zeisberg, E. M., Potenta, S., Xie, L., Zeisberg, M., and Kalluri, R. (2007). Discovery of endothelial to mesenchymal transition as a source for carcinoma-associated fibroblasts. Cancer Res. 67, 10123–10128. doi: 10.1158/0008-5472.Can-07-3127

PubMed Abstract | CrossRef Full Text | Google Scholar

Zeng, J., Chen, S., Li, C., Ye, Z., Lin, B., Liang, Y., et al. (2020). Mesenchymal stem/stromal cells-derived IL-6 promotes nasopharyngeal carcinoma growth and resistance to cisplatin via upregulating CD73 expression. J. Cancer 11, 2068–2079. doi: 10.7150/jca.37932

PubMed Abstract | CrossRef Full Text | Google Scholar

Zhai, J., Shen, J., Xie, G., Wu, J., He, M., Gao, L., et al. (2019). Cancer-associated fibroblasts-derived IL-8 mediates resistance to cisplatin in human gastric cancer. Cancer Lett. 454, 37–43. doi: 10.1016/j.canlet.2019.04.002

PubMed Abstract | CrossRef Full Text | Google Scholar

Zhang, B., Li, M., McDonald, T., Holyoake, T. L., Moon, R. T., Campana, D., et al. (2013). Microenvironmental protection of CML stem and progenitor cells from tyrosine kinase inhibitors through N-cadherin and Wnt–β-catenin signaling. Blood 121, 1824–1838. doi: 10.1182/blood-2012-02-412890

PubMed Abstract | CrossRef Full Text | Google Scholar

Zhang, D., Ding, L., Li, Y., Ren, J., Shi, G., Wang, Y., et al. (2017). Midkine derived from cancer-associated fibroblasts promotes cisplatin-resistance via up-regulation of the expression of lncRNA ANRIL in tumour cells. Sci. Rep. 7:16231. doi: 10.1038/s41598-017-13431-y

PubMed Abstract | CrossRef Full Text | Google Scholar

Zhang, H., Deng, T., Liu, R., Ning, T., Yang, H., Liu, D., et al. (2020). CAF secreted miR-522 suppresses ferroptosis and promotes acquired chemo-resistance in gastric cancer. Mol. Cancer 19:43. doi: 10.1186/s12943-020-01168-8

PubMed Abstract | CrossRef Full Text | Google Scholar

Zhang, H., Xie, C., Yue, J., Jiang, Z., Zhou, R., Xie, R., et al. (2017). Cancer-associated fibroblasts mediated chemoresistance by a FOXO1/TGFβ1 signaling loop in esophageal squamous cell carcinoma. Mol. Carcinog. 56, 1150–1163. doi: 10.1002/mc.22581

PubMed Abstract | CrossRef Full Text | Google Scholar

Zhang, L., Yao, J., Li, W., and Zhang, C. (2018). Micro-RNA-21 regulates cancer-associated fibroblast-mediated drug resistance in pancreatic Cancer. Oncol. Res. 26, 827–835. doi: 10.3727/096504017x14934840662335

PubMed Abstract | CrossRef Full Text | Google Scholar

Zhang, M. M., Di Martino, J. S., Bowman, R. L., Campbell, N. R., Baksh, S. C., Simon-Vermot, T., et al. (2018). Adipocyte-derived lipids mediate melanoma progression via FATP proteins. Cancer Discov. 8, 1006–1025. doi: 10.1158/2159-8290.Cd-17-1371

PubMed Abstract | CrossRef Full Text | Google Scholar

Zhang, Q., Yang, J., Bai, J., and Ren, J. (2018). Reverse of non-small cell lung cancer drug resistance induced by cancer-associated fibroblasts via a paracrine pathway. Cancer Sci. 109, 944–955. doi: 10.1111/cas.13520

PubMed Abstract | CrossRef Full Text | Google Scholar

Zhang, X., Chen, Y., Hao, L., Hou, A., Chen, X., Li, Y., et al. (2016). Macrophages induce resistance to 5-fluorouracil chemotherapy in colorectal cancer through the release of putrescine. Cancer Lett. 381, 305–313. doi: 10.1016/j.canlet.2016.08.004

PubMed Abstract | CrossRef Full Text | Google Scholar

Zhang, X., Tu, H., Yang, Y., Fang, L., Wu, Q., and Li, J. (2017). Mesenchymal stem cell-derived extracellular vesicles: roles in tumor growth, progression, and drug resistance. Stem Cells Int. 2017:1758139. doi: 10.1155/2017/1758139

PubMed Abstract | CrossRef Full Text | Google Scholar

Zhang, X., Tu, H., Yang, Y., Jiang, X., Hu, X., Luo, Q., et al. (2019). Bone marrow-derived mesenchymal stromal cells promote resistance to tyrosine kinase inhibitors in chronic myeloid leukemia via the IL-7/JAK1/STAT5 pathway. J. Biol. Chem. 294, 12167–12179. doi: 10.1074/jbc.RA119.008037

PubMed Abstract | CrossRef Full Text | Google Scholar

Zhang, Y., Guoqiang, L., Sun, M., and Lu, X. (2020). Targeting and exploitation of tumor-associated neutrophils to enhance immunotherapy and drug delivery for cancer treatment. Cancer Biol. Med. 17, 32–43. doi: 10.20892/j.issn.2095-3941.2019.0372

PubMed Abstract | CrossRef Full Text | Google Scholar

Zhao, J., Wang, H., Hsiao, C.-H., Chow, D. S. L., Koay, E. J., Kang, Y., et al. (2018). Simultaneous inhibition of hedgehog signaling and tumor proliferation remodels stroma and enhances pancreatic cancer therapy. Biomaterials 159, 215–228. doi: 10.1016/j.biomaterials.2018.01.014

PubMed Abstract | CrossRef Full Text | Google Scholar

Zheng, P., Chen, L., Yuan, X., Luo, Q., Liu, Y., Xie, G., et al. (2017). Exosomal transfer of tumor-associated macrophage-derived miR-21 confers cisplatin resistance in gastric cancer cells. J. Exp. Clin. Cancer Res. 36:53. doi: 10.1186/s13046-017-0528-y

PubMed Abstract | CrossRef Full Text | Google Scholar

Zhou, B., Sun, C., Li, N., Shan, W., Lu, H., Guo, L., et al. (2016). Cisplatin-induced CCL5 secretion from CAFs promotes cisplatin-resistance in ovarian cancer via regulation of the STAT3 and PI3K/Akt signaling pathways. Int. J. Oncol. 48, 2087–2097. doi: 10.3892/ijo.2016.3442

PubMed Abstract | CrossRef Full Text | Google Scholar

Zhou, S. L., Zhou, Z. J., Hu, Z. Q., Huang, X. W., Wang, Z., Chen, E. B., et al. (2016). Tumor-associated neutrophils recruit macrophages and T-Regulatory cells to promote progression of hepatocellular carcinoma and resistance to sorafenib. Gastroenterology 150, 1646.e17–1658.e17. doi: 10.1053/j.gastro.2016.02.040

PubMed Abstract | CrossRef Full Text | Google Scholar

Zhu, X., Shen, H., Yin, X., Yang, M., Wei, H., Chen, Q., et al. (2019). Macrophages derived exosomes deliver miR-223 to epithelial ovarian cancer cells to elicit a chemoresistant phenotype. J. Exp. Clin. Cancer Res. 38:81. doi: 10.1186/s13046-019-1095-1

PubMed Abstract | CrossRef Full Text | Google Scholar

Zou, F., Zhang, Z. H., Zhang, Y. T., Zhao, J. Q., Zhang, X. L., Wen, C. L., et al. (2017). Cancer-associated-fibroblasts regulate the chemoresistance of lung cancer cell line A549 via SDF-1 secretion. Zhonghua Zhong Liu Za Zhi 39, 339–343. doi: 10.3760/cma.j.issn.0253-3766.2017.05.004

PubMed Abstract | CrossRef Full Text | Google Scholar

Keywords: tumor microenvironment, antineoplastic drug resistance, cell-cell interplays, CAFs, TAMs, MSCs

Citation: Ni Y, Zhou X, Yang J, Shi H, Li H, Zhao X and Ma X (2021) The Role of Tumor-Stroma Interactions in Drug Resistance Within Tumor Microenvironment. Front. Cell Dev. Biol. 9:637675. doi: 10.3389/fcell.2021.637675

Received: 04 December 2020; Accepted: 19 April 2021;
Published: 20 May 2021.

Edited by:

Yong Song, Nanjing University, China

Reviewed by:

Hongzhi Du, Hubei University of Chinese Medicine, China
Yinlong Zhang, National Center for Nanoscience and Technology (CAS), China

Copyright © 2021 Ni, Zhou, Yang, Shi, Li, Zhao and Ma. This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.

*Correspondence: Xia Zhao, xia-zhao@126.com; Xuelei Ma, drmaxuelei@gmail.com

These authors have contributed equally to this work and share first authorship

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