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CCRL2 promotes antitumor T-cell immunity via amplifying TLR4-mediated immunostimulatory macrophage activation

Wei Yin, Yihong Li, Yan Song, J. Zhang, Chao Wu, Yu Chen, Ying Miao, Changdong Lin, Yuli Lin, Dapeng Yan, Jianfeng Chen, Rui He

2021Proceedings of the National Academy of Sciences70 citationsDOIOpen Access PDF

Abstract

Significance Macrophages play a key role in shaping tumor immunity. CCRL2 was originally cloned from LPS-stimulated macrophages; however, whether CCRL2 influences tumor immunity by regulating macrophage function remains unknown. In this study, we identify CCRL2 as a predictive indicator of robust antitumor immunity in human cancers and report the predominant expression of CCLR2 in TAM with immunostimulatory phenotypes. We also reveal the functional role of CCRL2 in potentiating antitumor immunity. Specifically, CCRL2 that is primarily induced by TLR4 agonists in turn interacts with TLR4 to facilitate its retainment in cell surface, thereby amplifying membrane TLR4-mediated downstream inflammatory signaling, finally leading to optimal activation of immunostimulatory macrophages and subsequent antitumor CD8 + T-cell responses.

Topics & Concepts

MacrophageImmunologyImmunityTLR4Cell mediated immunityBiologyImmune systemIn vitroGeneticsImmune Cell Function and InteractionImmunotherapy and Immune ResponsesImmune cells in cancer
CCRL2 promotes antitumor T-cell immunity via amplifying TLR4-mediated immunostimulatory macrophage activation | Litcius