AUTHOR=Bartneck Joschka , Hartmann Ann-Kathrin , Stein Lara , Arnold-Schild Danielle , Klein Matthias , Stassen Michael , Marini Federico , Pielenhofer Jonas , Meiser Sophie Luise , Langguth Peter , Mack Matthias , Muth Sabine , Probst Hans-Christian , Schild Hansjörg , Radsak Markus Philipp 

TITLE=Tumor-infiltrating CCR2+ inflammatory monocytes counteract specific immunotherapy

JOURNAL=Frontiers in Immunology

VOLUME=14

YEAR=2023

URL=https://www.frontiersin.org/journals/immunology/articles/10.3389/fimmu.2023.1267866

DOI=10.3389/fimmu.2023.1267866

ISSN=1664-3224

ABSTRACT=<p>Tumor development and progression is shaped by the tumor microenvironment (TME), a heterogeneous assembly of infiltrating and resident host cells, their secreted mediators and intercellular matrix. In this context, tumors are infiltrated by various immune cells with either pro-tumoral or anti-tumoral functions. Recently, we published our non-invasive immunization platform DIVA suitable as a therapeutic vaccination method, further optimized by repeated application (DIVA<sup>2</sup>). In our present work, we revealed the therapeutic effect of DIVA<sup>2</sup> in an MC38 tumor model and specifically focused on the mechanisms induced in the TME after immunization. DIVA<sup>2</sup> resulted in transient tumor control followed by an immune evasion phase within three weeks after the initial tumor inoculation. High-dimensional flow cytometry analysis and single-cell mRNA-sequencing of tumor-infiltrating leukocytes revealed cytotoxic CD8<sup>+</sup> T cells as key players in the immune control phase. In the immune evasion phase, inflammatory CCR2<sup>+</sup> PDL-1<sup>+</sup> monocytes with immunosuppressive properties were recruited into the tumor leading to suppression of DIVA<sup>2</sup>-induced tumor-reactive T cells. Depletion of CCR2<sup>+</sup> cells with specific antibodies resulted in prolonged survival revealing CCR2<sup>+</sup> monocytes as important for tumor immune escape in the TME. In summary, the present work provides a platform for generating a strong antigen-specific primary and memory T cell immune response using the optimized transcutaneous immunization method DIVA<sup>2</sup>. This enables protection against tumors by therapeutic immune control of solid tumors and highlights the immunosuppressive influence of tumor infiltrating CCR2<sup>+</sup> monocytes that need to be inactivated in addition for successful cancer immunotherapy.</p>