| Literature DB >> 33513345 |
Heng Lin1, Ilona Kryczek1, Shasha Li2, Michael D Green3, Alicia Ali4, Reema Hamasha4, Shuang Wei1, Linda Vatan1, Wojciech Szeliga1, Sara Grove1, Xiong Li1, Jing Li1, Weichao Wang1, Yijian Yan1, Jae Eun Choi5, Gaopeng Li1, Yingjie Bian1, Ying Xu1, Jiajia Zhou1, Jiali Yu1, Houjun Xia1, Weimin Wang1, Ajjai Alva4, Arul M Chinnaiyan6, Marcin Cieslik7, Weiping Zou8.
Abstract
Immunotherapy induces durable clinical responses in a fraction of patients with cancer. However, therapeutic resistance poses a major challenge to current immunotherapies. Here, we identify that expression of tumor stanniocalcin 1 (STC1) correlates with immunotherapy efficacy and is negatively associated with patient survival across diverse cancer types. Gain- and loss-of-function experiments demonstrate that tumor STC1 supports tumor progression and enables tumor resistance to checkpoint blockade in murine tumor models. Mechanistically, tumor STC1 interacts with calreticulin (CRT), an "eat-me" signal, and minimizes CRT membrane exposure, thereby abrogating membrane CRT-directed phagocytosis by antigen-presenting cells (APCs), including macrophages and dendritic cells. Consequently, this impairs APC capacity of antigen presentation and T cell activation. Thus, tumor STC1 inhibits APC phagocytosis and contributes to tumor immune evasion and immunotherapy resistance. We suggest that STC1 is a previously unappreciated phagocytosis checkpoint and targeting STC1 and its interaction with CRT may sensitize to cancer immunotherapy.Entities:
Keywords: PD-1; T cell immunity; calreticulin; checkpoint; dendritic cell; eat-me signal; macrophages; phagocytosis; stanniocalcin 1; tumor
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Year: 2021 PMID: 33513345 PMCID: PMC8044011 DOI: 10.1016/j.ccell.2020.12.023
Source DB: PubMed Journal: Cancer Cell ISSN: 1535-6108 Impact factor: 31.743