| Literature DB >> 33242418 |
Liwei Jiang1, Yi-Jun Wang1, Jing Zhao1, Mayuko Uehara1, Qingming Hou2, Vivek Kasinath1, Takaharu Ichimura3, Naima Banouni1, Li Dai1, Xiaofei Li1, Dale L Greiner4, Leonard D Shultz5, Xiaolong Zhang6, Zhen-Yu Jim Sun7, Ian Curtin8, Nicholas E Vangos8, Zoe C Yeoh8, Ezekiel A Geffken8, Hyuk-Soo Seo7, Ze-Xian Liu6, Gregory J Heffron9, Khalid Shah10, Sirano Dhe-Paganon7, Reza Abdi11.
Abstract
Cancer therapies kill tumors either directly or indirectly by evoking immune responses and have been combined with varying levels of success. Here, we describe a paradigm to control cancer growth that is based on both direct tumor killing and the triggering of protective immunity. Genetic ablation of serine protease inhibitor SerpinB9 (Sb9) results in the death of tumor cells in a granzyme B (GrB)-dependent manner. Sb9-deficient mice exhibited protective T cell-based host immunity to tumors in association with a decline in GrB-expressing immunosuppressive cells within the tumor microenvironment (TME). Maximal protection against tumor development was observed when the tumor and host were deficient in Sb9. The therapeutic utility of Sb9 inhibition was demonstrated by the control of tumor growth, resulting in increased survival times in mice. Our studies describe a molecular target that permits a combination of tumor ablation, interference within the TME, and immunotherapy in one potential modality. Published by Elsevier Inc.Entities:
Keywords: SerpinB9; antitumor immune response; cancer-associated fibroblasts; granzyme B
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Year: 2020 PMID: 33242418 PMCID: PMC7927154 DOI: 10.1016/j.cell.2020.10.045
Source DB: PubMed Journal: Cell ISSN: 0092-8674 Impact factor: 41.582