Reprogramming the tumor microenvironment leverages CD8+T cell responses to a shared tumor/self antigen in ovarian cancer

被引:5
|
作者
Mistarz, Anna [1 ,7 ]
Winkler, Marta [1 ]
Battaglia, Sebastiano [1 ,8 ]
Liu, Song [2 ]
Hutson, Alan [2 ]
Rokita, Hanna [3 ]
Gambotto, Andrea [4 ]
Odunsi, Kunle O. [5 ]
Singh, Prashant K. [6 ]
Mcgray, A. J. Robert [1 ]
Wang, Jianmin [2 ,9 ]
Kozbor, Danuta [1 ,10 ]
机构
[1] Roswell Pk Comprehens Canc Ctr, Dept Immunol, Buffalo, NY 14263 USA
[2] Roswell Pk Comprehens Canc Ctr, Dept Biostat & Bioinformat, Buffalo, NY 14263 USA
[3] Jagiellonian Univ, Fac Biochem Biophys & Biotechnol, PL-30387 Krakow, Poland
[4] Univ Pittsburgh, Dept Surg, Pittsburgh, PA 15261 USA
[5] Univ Chicago, Comprehens Canc Ctr, Chicago, IL 60637 USA
[6] Roswell Pk Comprehens Canc Ctr, Canc Genet & Genom, Buffalo, NY 14263 USA
[7] Jagiellonian Univ, Fac Biochem Biophys & Biotechnol, PL-30387 Krakow, Poland
[8] Johnson & Johnson, Janssen Pharmaceut Res & Dev, Spring House, PA 19002 USA
[9] Roswell Pk Comprehens Canc Ctr, Dept Biostat & Bioinformat, Buffalo, NY 14263 USA
[10] Roswell Pk Comprehens Canc Ctr, Dept Immunol, Buffalo, NY 14263 USA
来源
关键词
T-CELLS; CXCL12/CXCR4; BLOCKADE; CXCR4; ANTAGONIST; GROWTH; MACROPHAGES; FIBROBLASTS; EXPRESSION; STIMULATION; DYSFUNCTION;
D O I
10.1016/j.omto.2023.02.002
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Tumor antigen-driven responses to weakly immunogenic selfantigens and neoantigens directly affect treatment efficacy following immunotherapy. Using orthotopically grown SV40 T antigen+ ovarian carcinoma in antigen-naive wildtype or TgMISIIR-TAg-Low transgenic mice expressing SV40 T antigen as a self-antigen, we investigated the impact of CXCR4-antagonist-armed oncolytic virotherapy on tumor progression and antitumor immunity. Immunostaining and single-cell RNA sequencing analyses of the peritoneal tumor microenvironment of untreated tumors in syngeneic wildtype mice revealed the presence of SV40 T antigen-specific CD8+ T cells, a balanced M1/M2 transcriptomic signature of tumor-associated macrophages, and immunostimulatory cancer-associated fibroblasts. This contrasted with polarized M2 tumor-associated macrophages, immunosuppressive cancer-associated fibroblasts, and poor immune activation in TgMISIIR-TAg-Low mice. Intraperitoneal delivery of CXCR4antagonist-armed oncolytic vaccinia virus led to nearly complete depletion of cancer-associated fibroblasts, M1 polarization of macrophages, and generation of SV40 T antigen-specific CD8+ T cells in transgenic mice. Cell depletion studies revealed that the therapeutic effect of armed oncolytic virotherapy was dependent primarily on CD8+ cells. These results demonstrate that targeting the interaction between immunosuppressive cancer-associated fibroblasts and macrophages in the tolerogenic tumor microenvironment by CXCR4-A-armed responses and consequently increases therapeutic efficacy in an immunocompetent ovarian cancer model.
引用
收藏
页码:230 / 248
页数:19
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