TREM2 mediates MHCII-associated CD4+T cell response against gliomas

特雷姆2 胶质瘤 小胶质细胞 癌症研究 髓样 免疫系统 吞噬作用 生物 医学 髓系细胞 免疫学 炎症
作者
Jiaying Zheng,Lingxiao Wang,Shunyi Zhao,Wenjing Zhang,Yuzhou Chang,Aastha Dheer,Shan Gao,Shengze Xu,Katayoun Ayasoufi,Rawan Al‐kharboosh,Manling Xie,Aaron J. Johnson,Haidong Dong,Alfredo Quiñones‐Hinojosa,Long‐Jun Wu
标识
DOI:10.1101/2023.04.05.535697
摘要

Triggering receptor expressed on myeloid cells 2 (TREM2) was recently highlighted as a novel immune suppressive marker in peripheral tumors. The aim of this study was to characterize TREM2 expression in gliomas and investigate its contribution in glioma progression by using Trem2-/- mouse line. Our results showed that higher TREM2 expression was correlated with poor prognosis in glioma patients. Unexpectedly, TREM2 deficiency did not have a beneficial effect in a pre-clinical model of glioma. The increased TREM2 expression in glioma was likely due to increased myeloid cell infiltration, as evidenced by our single-cell analysis showing that almost all microglia and macrophages in gliomas were TREM2+. Furthermore, we found that deficiency of TREM2 impaired tumor-myeloid phagocytosis and MHCII presentation, and significantly reduced CD4+ T cells in tumor hemispheres. Our results revealed a previously unrecognized protective role of tumor-myeloid TREM2 in promoting MHCII-associated CD4+ T cell response against gliomas.
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