| Literature DB >> 28685773 |
Young-Hee Lee1, Natalia Martin-Orozco1,2, Peilin Zheng3,4,5, Jing Li6, Peng Zhang7, Haidong Tan8, Hyun Jung Park9, Mira Jeong10, Seon Hee Chang1, Byung-Seok Kim1, Wei Xiong4,5, Wenjuan Zang6, Li Guo11, Yang Liu7, Zhong-Jun Dong6, Willem W Overwijk12, Patrick Hwu12, Qing Yi13,14, Larry Kwak13,15, Zhiying Yang8, Tak W Mak16, Wei Li9, Laszlo G Radvanyi12,2, Ling Ni6, Dongfang Liu3,4, Chen Dong6.
Abstract
The interaction between tumor and the immune system is still poorly understood. Significant clinical responses have been achieved in cancer patients treated with antibodies against the CTLA4 and PD-1/PD-L1 checkpoints; however, only a small portion of patients responded to the therapies, indicating a need to explore additional co-inhibitory molecules for cancer treatment. B7-H3, a member of the B7 superfamily, was previously shown by us to inhibit T-cell activation and autoimmunity. In this study, we have analyzed the function of B7-H3 in tumor immunity. Expression of B7-H3 was found in multiple tumor lines, tumor-infiltrating dendritic cells, and macrophages. B7-H3-deficient mice or mice treated with an antagonistic antibody to B7-H3 showed reduced growth of multiple tumors, which depended on NK and CD8+ T cells. With a putative receptor expressed by cytotoxic lymphocytes, B7-H3 inhibited their activation, and its deficiency resulted in increased cytotoxic lymphocyte function in tumor-bearing mice. Combining blockades of B7-H3 and PD-1 resulted in further enhanced therapeutic control of late-stage tumors. Taken together, our results indicate that the B7-H3 checkpoint may serve as a novel target for immunotherapy against cancer.Entities:
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Year: 2017 PMID: 28685773 PMCID: PMC5539354 DOI: 10.1038/cr.2017.90
Source DB: PubMed Journal: Cell Res ISSN: 1001-0602 Impact factor: 25.617