| Literature DB >> 32376804 |
Kevin Van der Jeught1, Yifan Sun1, Yuanzhang Fang1, Zhuolong Zhou1, Hua Jiang2, Tao Yu1, Jinfeng Yang2, Malgorzata M Kamocka3, Ka Man So4, Yujing Li1, Haniyeh Eyvani1, George E Sandusky5, Michael Frieden1, Harald Braun6,7, Rudi Beyaert6,7, Xiaoming He8,9, Xinna Zhang1,10, Chi Zhang1,4,10, Sophie Paczesny2,10, Xiongbin Lu1,10.
Abstract
Immune checkpoint blockade immunotherapy delivers promising clinical results in colorectal cancer (CRC). However, only a fraction of cancer patients develop durable responses. The tumor microenvironment (TME) negatively impacts tumor immunity and subsequently clinical outcomes. Therefore, there is a need to identify other checkpoint targets associated with the TME. Early-onset factors secreted by stromal cells as well as tumor cells often help recruit immune cells to the TME, among which are alarmins such as IL-33. The only known receptor for IL-33 is stimulation 2 (ST2). Here we demonstrated that high ST2 expression is associated with poor survival and is correlated with low CD8+ T cell cytotoxicity in CRC patients. ST2 is particularly expressed in tumor-associated macrophages (TAMs). In preclinical models of CRC, we demonstrated that ST2-expressing TAMs (ST2+ TAMs) were recruited into the tumor via CXCR3 expression and exacerbated the immunosuppressive TME; and that combination of ST2 depletion using ST2-KO mice with anti-programmed death 1 treatment resulted in profound growth inhibition of CRC. Finally, using the IL-33trap fusion protein, we suppressed CRC tumor growth and decreased tumor-infiltrating ST2+ TAMs. Together, our findings suggest that ST2 could serve as a potential checkpoint target for CRC immunotherapy.Entities:
Keywords: Cancer immunotherapy; Colorectal cancer; Immunology; Inflammation; Macrophages
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Year: 2020 PMID: 32376804 PMCID: PMC7253019 DOI: 10.1172/jci.insight.136073
Source DB: PubMed Journal: JCI Insight ISSN: 2379-3708