- 1Department of Otolaryngology, Head and Neck Surgery, West China Hospital, West China Medical School, Sichuan University, Chengdu, Sichuan, China
- 2State Key Laboratory of Biotherapy, West China Medical School, Sichuan University, Chengdu, Sichuan, China
Negative checkpoint regulators (NCRs) reduce the T cell immune response against self-antigens and limit autoimmune disease development. V-domain Ig suppressor of T cell activation (VISTA), a novel immune checkpoint in the B7 family, has recently been identified as one of the NCRs. VISTA maintains T cell quiescence and peripheral tolerance. VISTA targeting has shown promising results in treating immune-related diseases, including cancer and autoimmune disease. In this review, we summarize and discuss the immunomodulatory role of VISTA, its therapeutic potential in allergic, autoimmune disease, and transplant rejection, as well as the current therapeutic antibodies, to present a new method for regulating immune responses and achieving durable tolerance for the treatment of autoimmune disease and transplantation.
Introduction
Immune checkpoints inhibitors transmit coinhibitory signals during T cell activation, thereby directly suppressing T cell responses (1). Coinhibitory molecules on T cells, including programmed Death-1 (PD-1), cytotoxic T lymphocyte antigen 4 (CTLA-4), T cell immunoglobulin and mucin domain 3 (Tim-3), Lymphocyte-activation gene 3 (Lag-3), and B and T lymphocyte attenuator (BTLA), can disrupt signaling mechanisms or induce negative intracellular signaling pathways on antigen-presenting cells (APCs) or other cells types (1, 2). Several immune-checkpoint regulator molecules are critical in modulating T cell responses and involved abnormally T cells response mediated inflammatory and autoimmunity diseases (3), which revitalized interest in utilizing antibodies against immunosuppress checkpoint regulators to counter the effects of these molecules.
V-domain immunoglobulin suppressor of T-cell activation (VISTA) is a novel immune inhibitory molecule of the B7 family (4) that can negatively regulate immune responses, maintains peripheral tolerance, and control autoimmunity (5, 6). VISTA is revealed to function as an immune checkpoint in multiple mouse immune pathology diseases models, such as graft-versus-host disease (GVHD), rheumatoid arthritis (RA), asthma, and experimental allergic encephalomyelitis (EAE), and VISTA-deficient mice increase susceptibility to developing autoimmunity (7). The multi-faceted role of VISTA in regulating immune responses has suggested the utility of VISTA as a potential reagent in the prevention or even therapeutic cure of allergic, autoimmune disease and transplant rejection (7–9).
This review aims to illuminate the expression and biological effects of VISTA and discuss the current research progress in preclinical studies on allergies, autoimmune diseases, and organ transplantation using VISTA. In addition, VISTA’s potential as an immune modulator encourages further research on current antibodies, which can control immune responses and achieve durable tolerance for the treatment of autoimmune disease and transplantation.
The structure and expression of VISTA
VSITA, also known as PD-1H (10), c10orf54 (11), DD1α (12), Dies1 (13), is a type I transmembrane protein on chromosome 10q22.1 containing 311 amino acids (14). VISTA comprises an extracellular IgV domain, a stalk segment, a transmembrane region, and a conserved cytoplasmic tail. The structure of VISTA shares similarities with PD1, CD28, and CTLA4 (15), but the cytoplasmic tail of VISTA lacks a classic immunoreceptor tyrosine-based inhibition motif (ITIM) or immunoreceptor tyrosine-based activation motif (ITAM) (4). VISTA is conserved with 76% identity between humans and mice. Interestingly, the cytoplasmic tail shares 90.6% identity between humans and mice, indicating a highly conserved functional role, whereas the cytoplasmic tail of PD1 between humans and mice only shares 59% identity (4).
VISTA is expressed in several organs and tissues, including the spleen, heart, kidney, thymus, brain, and bone marrow (14). Expression of VISTA is constitutive and limited to hematopoietic cells; there is a significant expression of VISTA in monocytes, macrophages, neutrophils, and dendritic cells (DCs), as well as on all types of T cells, including naïve CD4 and CD8 T cells and regulatory T cells (Tregs), both in human (16) and mice (10, 14), but not on B cells. Interestingly, VISTA is not only expressed on the cell surface, but also expressed in the intracellular of myeloid compartment (17). B lymphocytes, natural killer cells (NK), and other lymphocytes expressed by mice and humans have almost no expression of VISTA (14). VISTA is also expressed in various types of tumors, including ovarian and endometrial cancer (18), prostate cancer (19), hepatocellular carcinomas (20), pancreatic cancer (21), gastric carcinoma (22), and colorectal carcinoma (23). In the tumor microenvironment, VISTA is highly expressed on myeloid-derived suppressor cells (MDSC) and regulates their effector functions (24, 25).
VISTA binding partners
As VISTA contains two potential protein kinase C binding sites in its cytoplasmic tail domain (14), that could function as docking sites, suggesting that it is a coinhibitory molecule with dual functions as both receptor and ligand (11). VISTA can function as a coinhibitory receptor on T cells to suppress naive T cell response. VISTA expressed in APCs interacts with certain T cell receptors to inhibit T cell activation and proliferation (11). Several researchers have identified a potential VISTA-binding ligand, but the counterreceptor of VISTA remains elusive. There are two confirmed ligands of VISTA with immunosuppressive functions; one is VSIG3 (V-Set and Immunoglobulin domain containing 3) and PSGL1 (P-selectin glycoprotein ligand 1) (26, 27). VISTA interacts with VSIG3 at physiological PH environment, while at acidic pH environment to PSGL-1, both interactions led to the suppression of T cell function (26, 27) (Figure 1).
Figure 1 VISTA binding partners. VSIG3 interaction with VISTA on T cells suppresses T cell activation and proliferation. VISTA activity decreases reducing the production of several cytokines, including IFN-γ, IL-2, IL-17, CCL3, CCL5, and CXCL11. VISTA expressed on tumor cells, tumor-associated macrophages (TAMs) or MDSCs can bind to PSGL-1 on T cells at pH 6.0, and promoting T cell exhaustion.
Wang and colleagues reported that VSIG3 is a ligand of VISTA that inhibits the proliferation and functions of human T cells. The expression of VSIG3 is primarily observed in non-hematopoietic cells (26). VISTA interacts with VSIG3 in vitro, reducing the production of several cytokines, including IFN-γ, IL-2, IL-17, CCL3, CCL5, and CXCL11 (26). However, VSIG3 expression is undetectable in hematopoietic cells, and the physiological relevance of VISTA-VSIG3 interaction in vivo remains to be validated. Korman et al. identified PSGL-1 as a VISTA binding partner via histidine residues within the extracellular domain (27), and the interaction is regulated by the pH in microenvironment (27). VISTA interacts with PSGL-1 in vitro and in vivo, suppressing T-cell response at acidic pH 6.0 in the tumor microenvironment (28). Unlike VSIG3, PSGL-1 is expressed on a range of hematopoietic cells, with a lower expression on B cells and microvascular endothelial cells (29, 30). The functional binding of VISTA and PSGL-1 is regulated by tyrosine sulfation and glycosylation (31, 32). PSGL-1 are highly expressed in macrophages, granulocytes, microglia (17), and endothelial cells (28). There is a possibility that VISTA may have multiple binding partners. VSIG8, Galectin 9, and NSC622608 have been reported to bind to VISTA in addition to these two ligands, but further research is required to verify their functional binding (28, 33, 34).
Roles of VISTA in immunity interactions
Since VISTA is expressed across allergies, autoimmune diseases, and organ transplantation, and therapeutic agents are being developed to target VISTA, it is crucial to determine which cells are affected by VISTA expression.
Age and gender
VISTA-deficient mice demonstrate an age-related proinflammatory signature (35). VISTA-deficient mice showed autoimmune defects apparent in the aged female mice and an accumulation of anti-nuclear and anti-dsDNA antibodies in the serum, spontaneous glomerulonephritis, and inflammatory phenotypes in the skin, eyes, and ears (12, 35). Interestingly, female animals are substantially more sensitive to the disease in various animal autoimmune disease models, including SLE (36). Similarly, extremely high gender bias (9:1) also has been described in humans for systemic autoimmune diseases (37).
T lymphocytes
VITSA is essential to maintain peripheral homeostasis of T cells. VISTA-deficient mice exhibit less peripheral T cell deletion and leading to the development of autoimmune phenotypes (5, 7). The transcriptomic analysis of T cells from VISTA-deficient mice demonstrates the importance of VISTA in maintaining naïve T cell quiescence and in activating T cells at early stage (5). Many studies suggest that VISTA on both T cells and APCs negatively regulates T cell responses via specific pathways, by acting as a ligand or a receptor. As a receptor on T cells, VISTA can function independently of APCs to negatively regulate T cell responses, as VISTA agonistic suppresses antigen-specific T cell proliferation when activated by VISTA-deficient APCs (2). In addition, VISTA-Ig fusion protein can inhibit T cell proliferation and reduce cytokine production.
Several experimental settings have explored the involvement of VISTA in T helper type 1 (Th1), type 2 (Th2), and type 17 (Th17) mediated immune responses. Most research has demonstrated that VISTA mediates immune responses mediated by Th1 and Th17 cells. Reducing VISTA expression can facilitate the expansion and differentiation of Th1 and Th17 T cells (38). Psoriasiform dermatitis is exacerbated by VISTA deficiency, which increases inflammatory responses in DCs, T cells, and Th17 cells (39). Consistently, murine VISTA knockout models raise susceptibility to develop experimental autoimmune encephalomyelitis that has been reported to be characterized by a Th1/Th17 response (40). The DC in VISTA deficient mice produces more IL-23, which further augments the production of IL17a by Th17 and γδ T cells (40). Compared to wild-type induced Tregs (iTregs), VISTA deficient mice have higher Th17 and Th1 cell formation rates during inflammation, which indicates that VISTA deficient mice have a more reactive T cell response (41). In addition, VISTA blockade or deficiency of preferentially activated CD8+ T cells, leading to secretion of IFN-γ may influence Th2 cell proliferation. VISTA was demonstrated to negatively inhibit the production of allergen-specific Th2 cells and Th2-mediated antibody secretion (42).
Like most other NCRs, VISTA is highly expressed in tumor-infiltrating Tregs and could suppress tumor-specific immunity. VISTA may also be involved in the differentiation and suppressive function of Treg, both as a receptor on T cells and as a ligand expressed by Tregs. Researchers have found that VISTA can induce and differentiate human and murine Treg cells (2). A reduced ability to convert T cells into iTregs is observed in mice lacking VISTA, but naturally occurring Tregs (nTregs) generation is unaffected (41). Moreover, VISTA blockade decreases the generation of tumor-specific Treg and reverses Treg-mediate suppression (16). However, VISTA blockade also increases T cell proliferation even in the absence of Tregs, indicating that there are other pathways that may involve in Treg mediated suppression (43).
Myeloid compartments
Human and mouse CD11bHi myeloid cells, including monocytes, macrophages, granulocytes, and myeloid dendritic cells, express VISTA at high levels; it is conceivable that VISTA expression may also correlate with an immune response (14, 42, 44). In various mouse models of inflammation, such as psoriasis (39), antibody-induced arthritis (45), experimental asthma (46), and lupus nephritis (47), VISTA deficient mice exhibit increased proinflammatory cytokines derived from T cells and myeloid compartments. The transient overexpression of VISTA in human monocytes increases cytokine secretion on protein level and mRNA, such as IL-1β, IL-6, IL-8, and TNFα (44, 48). VISTA is highly expressed by monocytes isolated from chronically HIV-positive individuals and elevated levels of the same cytokines (44). Deleting the cytoplasmic domain of VISTA abolishes this activity, suggesting that VISTA regulates the activation of myeloid cells (44). Further research is needed to explore VISTA’s downstream signaling role in myeloid cells.
Additionally, VISTA is a P53 regulated surface receptor, expressed on both macrophages and neutrophils, and is essential for dead cell clearance (12). Neutralizing VISTA on macrophages reduced neutrophil efferocytosis in vitro (49). In a murine model of bacterial pneumonia, the distribution of VISTA is redirected from the macrophage-neutrophil interaction site to a more disorganized, diffuse surface expression around the macrophage cell and influences the efferocytosis process (49). Additionally, VISTA regulates macrophage functions, influences the M1 (classical) and M2 (alternative) reprogramming of macrophages, and controls the magnitude of innate inflammation in vivo (50). Mohamed et al. found that VISTA agonists promote the production of IL-10, miR-221, A20, immune response gene 1 (IRG1), and MerTK, which are involved in both M2 polarization and LPS tolerance, and reduced mediators of M1 polarization, including IFN regulatory factor 5 (IRF5) and IRF8, at transcriptional and protein levels (50). In addition, Nzeteu et al. found that activated M2 macrophages release significantly more VISTA than activated M1 macrophages (51).
Intriguingly, VISTA deficiency did not lead to a severe systemic autoimmune disorder, indicating that other immunoregulatory molecular, such as PD-1, CTLA-4, B7-H3, and B7-H4, might compensate for the VISTA genetic deficiency and mitigated the development of inflammation and autoimmunity induced by genetic loss of VISTA (5).
VISTA in allergic, autoimmune disease and transplant rejection
Recent evidence suggests that VISTA is also closely associated with allergic reactions, autoimmune diseases, and transplant rejection via multiple inhibitory mechanisms, which will be discussed in the following (Table 1). It is noteworthy that VISTA is also highly expressed in placental tissues (54). Normal pregnancies prefer a relatively immunosuppressive environment to tolerate fatal antigens, and the acidic environment caused by mild hypoxia may enhance the immunosuppressive activity of VISTA (54, 55). Therefore, VISTA in decidual immune cells can regulate maternal-fetal immunity (54). Research on VISTA’s role in maternal-fetal tolerance is also needed.
VISTA in allergic diseases
VISTA deficiency and blocking led to a significant increase in infiltrating inflammation in the airways with massive eosinophils in the experimental asthma model induced by OVA (46). VISTA KO mice exhibit increased amounts of Th2-type cytokines, including IL-5 and IL-13, as well as innate inflammatory cytokines, such as MCP-1, TNF-α, and IL-6. VISTA KO mice show a significant reduction in pulmonary CD4+ Foxp3+ Tregs during asthma induction. In addition, VSITA agonist mAb 4C11 suppressed pulmonary inflammation (46). Also, another VISTA antagonist (MIH63) increased Th2-type cytokine production in mice (42). Treatment with the VISTA antagonist (MIH63) during allergen sensitization elevated the IL-13 expression but did not increase the number of eosinophils and asthmatic responses. In contrast, MIH63 treatment during allergen challenge increased IL-4, IL-5, and IL-13 production and accelerated asthmatic responses (42). The results indicate that VISTA is crucial for modulating asthmatic responses (42, 46).
Sibaud et al. found that patients with melanoma given anti-PD-1/PD-L1 therapy were more likely to develop multiple dermatological complications, suggesting that immune checkpoint inhibitors may play important roles in the regulation of skin inflammation and autoimmunity (56). Consistent with this, one line of evidence has shown that VISTA is important in the maintenance of skin homeostasis and inflammation (52). It has been demonstrated that anti-VISTA mAbs can effectively inhibit allergic airway disease and allergic dermatitis (8, 46). T Ohno et al. analyzed the roles of VISTA in allergic skin inflammation using a murine 2,4-dinitro-1-fluorobenzene-induced contact hypersensitivity model. It was found that treatment with anti-mouse VISTA mAb (MIH63) (52, 57) at sensitization, but not at challenge, significantly boosted ear swelling and elevated IFN-γ and TNF-α secretion (52). Further analysis of draining lymph nodes revealed that VISTA antagonist treatment greatly increased the proportions of CD8+ CD25+ T cells, CD4+ IFN-γ+ T cells, and CD8+ IFN-γ+ T cells, and further increased both CD44high fractions in CD8+ T cells, but not affect the proportion of Foxp3+ Tregs (43, 52). Guo et al. found that VISTA-Ig can successfully alleviate erythema, a horny substance of allergic dermatitis mice (8). As a result, fewer inflammatory cells can be infiltrated, and inflammatory cytokines and IgE are produced (8).
It has been reported that human VISTA-Ig inhibits the proliferation of T cells and reduces cytokine production in T cells (16). However, the detailed role of VISTA in human skin diseases remains to be uncovered. Furthermore, the treatment with VISTA antagonist during the sensitization and challenge stage shows opposite results in the experimental asthma model, and the allergic skin inflammation model still needs further exploration. Accordingly, these observation raises the possibility that the administration of VISTA agonistics could be beneficial in steroid-resistant asthmatic patients and allergic dermatitis patients.
VISTA in autoinflammation and autoimmunity diseases
Increasingly studies have focused on the relationship between VISTA expressions and autoimmune diseases, such as SLE and RA. It has been discovered that VISTA deletion causes spontaneous autoimmunity and clinically obvious organ-specific autoimmune disease (7). Our discussion will focus on the role of VISTA in autoinflammation and autoimmunity disease, which may subsequently facilitate establishing the rationale for therapeutically enhancing VISTA-mediated pathways to benefit the treatment of multiple autoinflammatory and autoimmune disorders.
Systemic lupus erythematosus
Sabrina et al. found that patients with systemic lupus erythematosus and discoid lupus erythematosus (DLE) and autoimmune-prone MRL/lpr mice have up-regulated VISTA expression (58). They interbred VISTA-deficient mice with Sle1.Sle3 mice, and analyzed the impact of VISTA deficiency on lupus development in that lupus-prone mouse strain. They found that Sle1.Sle3 VISTA−/− mice showed enhanced CD4+ T cells and myeloid compartment activation and increased secretion of proinflammatory cytokines, chemokines, and interferon (IFN)–regulated genes associated with SLE, including IFNα, IFNγ, tumor necrosis factor, interleukin-10, and CXCL10 (58). A feature of lupus lesions from VISTA KO mice is pDC clustering, and neutrophils infiltrate the skin before clinically evident disease, and subsequently develop more severe systemic lupus erythematosus and inflammatory arthritis (48). An agonistic VISTA antibody can consistently inhibit T cell, pDC, and neutrophil function, suppressing autoimmune lupus in MRL/lpr mice (7). Meanwhile, the treatment with a VSITA-blocking antibody (13F3) exacerbates the progression of lupus and increases amounts of inflammatory myeloid cells and activated T cells (48). Notably, no difference was observed in total anti-dsDNA antibodies, anti-dsDNA-IgG antibody titers, dsDNA-IgM antibodies, or IgG, IgM deposition in the kidney, suggesting that VISTA has little effect on B cells. These findings suggest that VISTA activation could effectively treat systemic lupus erythematosus.
Rheumatoid arthritis
SLE was exacerbated by deleting VISTA, and VISTA agonist alleviated autoimmune lupus. However, different disease models exhibit opposite effects. For example, rheumatoid arthritis is also a chronic autoimmune inflammation that destroys cartilage, tendon, and bone in particular joints (56, 59). VISTA is expressed in the synovial tissue of joints in healthy and RA patients. By contrast, in a mouse model of collagen antibody-induced arthritis (CAIA), Ceeraz et al. (45) found that both VISTA gene knockout and specific VISTA-blocking antibody (8G8) modulated macrophage responses to immune complexes, significantly induced resistance to arthritis in mice and reduced arthritic inflammation. In addition, it was demonstrated that VISTA deficiency impaired responses of myeloid cells to C5a and regulated macrophage reactions to simulated immune complexes (45). Researchers speculated that it might be related to the type of mouse model and monoclonal antibody used in this study, as well as the type of immune cells involved in the occurrence of RA and, as in another case of CAIA, anti-VISTA antibody (MH5A) greatly reduced arthritic symptoms and joint damage (10). Therefore, future studies may consider selecting other RA models and mAb to further clarify the role of VISTA in the occurrence and development of RA.
Psoriasis
VISTA also has an inhibitory effect on the occurrence and development of psoriasis. In the imiquimod (IMQ)-induced psoriasis model, VISTA deficiency enhanced the production of IL17 by both γδ T cells and CD4+ Th17 cells and suppressed IMQ-induced TLR7 signaling and IL-23 production, resulting in exacerbated psoriasiform inflammation (40). These results reveal the anti-inflammatory role of VISTA through regulating the IL-23/IL-17 inflammatory axis, leading to the elevated level of inflammatory mediators in the skin and serum, including IL-1β, IL-6, IL-17A, IL-22, IL-23, IFN-γ, TNF-α, and CXCL2 (40).
VISTA and allogeneic transplantation
Organ transplantation is still challenging in clinical practice due to allogenic transplant rejection and Graft versus host disease. Therefore, numerous researchers are testing the clinical feasibility of targeting immunomodulatory molecules to prevent GVHD and prolong organ transplant survival.
GVHD is a reaction of activated allogeneic or major histocompatibility complex (MHC) mismatched T cells directed against host tissues, which may result in wide tissue damage, increasing the risk of metabolic disorder, opportunistic infection, and malignancy, and generally require immune suppression (11, 60). GVHD is commonly found in allogeneic hematopoietic cell transplantation for treating hematologic malignancies and in the setting of solid organ transplantation. Flies et al. found that VISTA-/- T cells induce exacerbated graft-versus-host disease compared to wild-type T cells and found the immunosuppressive impact of VISTA agonists in acute GVHD (11). By immunohistochemistry analysis, they found that the VISTA agonists (MH5A) can greatly reduce infiltrating T cells and suppress T cell activation in all GVHD target organs, such as the liver, spleen, kidney, and lung (2, 11). In addition, the VISTA agonists targeting VISTA on donor T cells can prevent GVHD (10).
Tomoyuki et al. (9) examined the role of VISTA in the immune-privilege status of corneal allotransplantation and allospecific anterior chamber-associated immune deviation (ACAID). The researchers found that VISTA-mediated immunomodulation protects corneal allografts from rejection and promotes survival. Two possible mechanisms are explored in this study. One was that VISTA is involved in the induction of donor-specific ACAID, that antigens-specific systemic immune tolerance to eye-derived antigens via splenic CD8+ CD103+ T regulatory cells (9). Additionally, they found that the corneal VISTA mediates immune suppression and reduces inflammatory cells within the eyes.
VISTA may contribute to GVHD and allograft rejection, and forced expression of VISTA may be a potential therapeutic strategy for conferring an immune-privileged status to suppress GVHD allograft rejection. However, the precise mechanism of VISTA in the modulation of T-cell response remains elucidated. Therefore, studies are needed to determine the signaling pathways mediated by VISTA on APCs and T cells, which will facilitate manipulation of the immune system for maintaining tolerance and graft survival with the least side effects.
VISTA in other CNS inflammation and diseases
Microglia, a major myeloid cell in the central nervous system (CNS). VISTA is most abundantly expressed by mouse and human microglia and involved in the immune response of microglia (43, 61). Therefore, understanding the role of VISTA in CNS inflammation and diseases is important. In accordance with SLE, anti-VISTA Ab administration in vivo enhanced disease progression in a passive EAE model. Furthermore, VISTA-deficient mice significantly enhanced the development and progression of EAE on a disease-prone transgenic background, suggesting that VISTA deficiency overcame additional immune-regulatory mechanisms, leading to elevated activated encephalitogenic T cells in the periphery and promoting its infiltration into the central nervous system (35).
As the VISTA may be involved in immune surveillance and uptake of apoptotic neurons or other debris by microglia (12, 61). Borggrewe et al. (62) summarized the role of VISTA in CNS inflammation, aging, and neurodegenerative diseases. The expression of VISTA by microglia is consistently decreased in neurodegenerative diseases (NDD), including Alzheimer’s disease, frontotemporal dementia, Parkinson’s disease, and amyotrophic lateral sclerosis. Reduction in VISTA expression during NDD leads to elevated production of cytokines and inhibits the clearance of cell debris which might enhance neuroinflammation (12, 40, 61).
VISTA expression consistently decreases in chronic active multiple sclerosis (MS) lesions and MS mouse model (61). Microglia VISTA slightly decreases in MS white matter, whereas there is no significant difference in MS grey matter (63, 64). The loss of VISTA expression on microglia in MS may exacerbate the activation of infiltrating T cells in the lesion, further enhancing inflammation and tissue destruction (65). Microglia also involves various CNS diseases, including stroke and Purkinje cell degeneration. The expression of VISTA by microglia is reduced 2-fold in the stroke murine model (62). Although inhibiting the activation of microglia during stroke facilitate to produce beneficial outcomes, microglial activation is also critical to counteract neuronal death and enhance neurogenesis and angiogenesis (62, 66).
Alzheimer’s and Parkinson’s disease may develop due to reduced VISTA expression in microglia during aging. For example, in mice, VISTA expression is reduced in microglia in aged mice compared with younger mice. And individuals > 50 years of age show a slight increase in VISTA expression compared with those < 50 years (62).
VISTA and viral infection
VISTA could also impact human immunodeficiency virus (HIV)-induced immune activation and T-cell response. Monocytes from HIV-infected subjects show increased expression of VISTA, which correlated with increased cytokine mRNA expression such as IL-1β, IL-6, IL-8, IL-10, and TNF-α, and immune activation (44), and these results indicated that VISTA might play a critical role in regulating the immune response in HIV infection. Additionally, VISTA may induce phagocytosis of HIV-infected T cells and subsequent upregulation of apoptosis (67). VISTA overexpression on both phagocytes and HIV-infected CEM-SS T cells facilitated phagocytosis (66). Moreover, it has been suggested that CXCL10 might serve as a prognostic biomarker and an essential pathogenic mediator of COVID-19 in recent studies (68, 69). The potential immunoregulatory role of VISTA in COVID-induced inflammation has also been explored as the anti-VISTA mAb suppresses CXCL10. Enrichment analysis of the COVID-19 immune profile indicates that anti-VISTA agonists may suppress the COVID-19 inflammatory signature, as the VISTA agonist downregulated almost 40% of COVID-19 hallmark immune genes (53). However, The underlining mechanism is still unknown, which could be related to VISTA agonist’s reduction of FcgRIIIa, as the Fc receptor responses have been reported as an immunopathologic feature of COVID-19 infection (53). The impact of VISTA on myeloid chemotaxis also makes it a promising target in COVID-19 cytokine storm management. In addition, heightened cytokine production from myeloid cells likely contributes to cytokine-release syndrome (CRS) induced by CAR-T cell therapy, and VISTA agonistic may ameliorate the innate inflammation of the CAR-T-induced CRS (53). Meanwhile, VISTA agonists likely would exert minimal inhibitory impact on activated CAR-T cells directly (53). However, there are limited numbers of studies on viral infection and VISTA biology, which topic remains largely unexplored.
Targeting VISTA in autoimmunity
Multiple functional outcomes of VISTA modulation are plausible in autoimmune diseases. VISTA antibodies can be divided into agonistic or antagonistic antibodies according to their function. VISTA agonistics has been shown to limit immune response and suppress proinflammatory cytokine production in several mice autoimmune diseases models, such as EAE, murine lupus nephritis, K/BxN arthritis, IMQ-induced psoriasis, and GVHD (5, 10). VISTA agonist mAb, such as MH5A (7, 10, 11) and 4C11 (46). Using these VISTA antagonistic in mice, such as 13F3 (14, 43), and MIH63 (42) exacerbates the severity of the allergy and autoimmune diseases, including asthma and EAE. On the contrary, VISTA antagonistic 8G8 suppresses the collagen antibody-induced arthritis (45). Researchers have no consensus regarding the exact function of the MH5A clone (70). MH5A clone acts as an agonist in the GVHD model and autoimmune lupus in MRL/lpr mice, whereas in the case of CAIA, Ceeraz et al. used it as an antagonist to reduce joint inflammation (45). The exact epitopes and properties involved with different monoclonal antibody against VISTA may account for these apparent various results (71).
Importantly, VISTA may also be involved in a large variety of functions, including phagocytosis, cytokine response, and chemotaxis, which make it complex to predict the outcome of VISTA modulation. Moreover, systemically using anti-VISTA antibodies may impact the immune function unpredictably. Therefore, it urges us to explore precise therapeutic antibodies which target distinct epitopes. In addition, an innovative strategy for engineering pH-selective anti-VISTA antibodies has been developed, targeting only the PH- dysregulation sites.
Conclusions
VISTA is a critical immune-checkpoint regulator that maintains peripheral tolerance and controls autoimmunity. Recent advances in targeting VISTA have shown promising results in immune-related diseases such as cancer and autoimmunity. VISTA-Ig and genetic VISTA ablation promotes proinflammatory cytokine production and leads to a susceptible condition under which autoimmune diseases are more likely to develop. VISTA manipulation or targeting to enhance or suppress its activity may offer promising therapeutic approaches for allergic, autoimmune disease and transplantation. The knowledge gap concerning VISTA binding partners is a critical limiting step in developing targeted therapy. Identifying VISTA’s binding partner is critical for clinical benefits and will further offer insight into the cellular and molecular immunomodulatory mechanisms of VISTA signaling. An in-depth understanding of VISTA’s immunomodulatory mechanisms has provided exceptional opportunities to therapeutically target or manipulate VISTA and design synergistic combination therapies for tolerance maintenance in allergic and autoimmune diseases and organ transplants.
Author contributions
All authors listed have made a substantial, direct, and intellectual contribution to the work and approved it for publication.
Funding
This work was supported by a grant from the Science and Technology Department of Sichuan Province, P. R. China (2022NSFSC0851&2022NSFSC0847).
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.
Publisher’s note
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Abbreviations
NCRs, Negative checkpoint regulators; VISTA, V-domain Ig suppressor of T cell activation; PD-1, Programmed Death-1; CTLA-4, Cytotoxic T lymphocyte antigen 4; Tim-3, T cell immunoglobulin and mucin domain 3; Lag-3, Lymphocyte-activation gene 3; BTLA, B and T lymphocyte attenuator; APCs, Antigen-presenting cells; GVHD, Graft-versus-host disease; SLE, Systemic lupus erythematosus; RA, Rheumatoid arthritis; EAE, Experimental allergic encephalomyelitis; ITIM, Immunoreceptor tyrosine-based inhibition motif; ITAM, Immunoreceptor tyrosine-based activation motif; DCs, Dendritic cells; Tregs, Regulatory T cells; MDSC, Myeloid derived suppressor cells; NK, Natural killer; VSIG3, V-Set and Immunoglobulin domain containing 3; PSGL1, P-selectin glycoprotein ligand 1; Th1, T helper type 1; iTregs, Induced Tregs; nTregs, Naturally occurring Tregs; IRG1, Immune response gene 1; IRF5, IFN regulatory factor 5; DLE, Discoid lupus erythematosus; CAIA, Collagen antibody-induced arthritis; MHC, Major histocompatibility complex; ACAID Anterior chamber-associated immune deviation; CNS, Central nervous system; NDD, Neurodegenerative diseases; MS, Multiple sclerosis; HIV, Human immunodeficiency virus; CRS, Cytokine-release syndrome.
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Keywords: V-domain Ig suppressor of T cell activation, VISTA, allergy, autoimmune disease, transplantation
Citation: Zheng M, Zhang Z, Yu L, Wang Z, Dong Y, Tong A and Yang H (2023) Immune-checkpoint protein VISTA in allergic, autoimmune disease and transplant rejection. Front. Immunol. 14:1194421. doi: 10.3389/fimmu.2023.1194421
Received: 27 March 2023; Accepted: 30 May 2023;
Published: 26 June 2023.
Edited by:
Qi Wang, Huazhong University of Science and Technology, ChinaReviewed by:
Ganesan Ramamoorthi, Moffitt Cancer Center, United StatesElizabeth Nowak, Dartmouth College, United States
Copyright © 2023 Zheng, Zhang, Yu, Wang, Dong, Tong and Yang. 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: Hui Yang, yh8806@163.com; Aiping Tong, aipingtong@scu.edu.cn