Single-cell RNA sequencing reveals the suppressive effect of PPP1R15A inhibitor Sephin1 in antitumor immunity

单细胞RNA测序揭示了PPP1R15A抑制剂Sephin1在抗肿瘤免疫中的抑制作用

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作者:Rongjing Wang ,Yuchao Zhang ,Shiwei Guo ,Siyu Pei ,Wei Guo ,Zhenchuan Wu ,Hailong Wang ,Minghui Wang ,Yizhe Li ,Yufei Zhu ,Ling-Hua Meng ,Jingyu Lang ,Gang Jin ,Yichuan Xiao ,Landian Hu ,Xiangyin Kong

Abstract

Protein phosphatase 1 regulatory subunit 15A (PPP1R15A) is an important factor in the integrated stress response (ISR) in mammals and may play a crucial role in tumorigenesis. In our studies, we found an inhibitor of PPP1R15A, Sephin1, plays a protumorigenic role in mouse tumor models. By analyzing the single-cell transcriptome data of the mouse tumor models, we found that in C57BL/6 mice, Sephin1 treatment could lead to higher levels of ISR activity and lower levels of antitumor immune activities. Specifically, Sephin1 treatment caused reductions in antitumor immune cell types and lower expression levels of cytotoxicity-related genes. In addition, T cell receptor (TCR) repertoire analysis demonstrated that the clonal expansion of tumor-specific T cells was inhibited by Sephin1. A special TCR + macrophage subtype in tumor was identified to be significantly depleted upon Sephin1 treatment, implying its key antitumor role. These results suggest that PPP1R15A has the potential to be an effective target for tumor therapy.

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