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APOE 抑制增强了癌症的免疫检查点治疗。

Inhibition of APOE potentiates immune checkpoint therapy for cancer.

机构信息

Department of Oncology, The First Affiliated Hospital of Nanjing Medical University, Nanjing, Jiangsu, China.

Department of General Surgery, The First Affiliated Hospital of Nanjing Medical University, Nanjing, Jiangsu, China.

出版信息

Int J Biol Sci. 2022 Aug 15;18(14):5230-5240. doi: 10.7150/ijbs.70117. eCollection 2022.

DOI:10.7150/ijbs.70117
PMID:36147474
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9461658/
Abstract

Checkpoint immunotherapy is capable of unleashing T cells for controlling tumor, whereas it is destroyed by immunosuppressive myeloid cell. Apoprotein E (APOE) refers to a ligand in terms of the members of low-density lipoprotein (LDL) receptor family for mediating Apoprotein B-involving atherogenic lipoprotein clearance. Besides, tumor-infiltration macrophage can express APOE. The present study reported Apoe mice to exhibit higher resistance toward the development of three types of carcinomas as compared with mice with wild type and to have greater responses to αPD-1 (anti-PD-1) immunotherapy. Moreover, treatment by exploiting APOE inhibitor (COG 133TFA, αAPOE) was capable of curbing tumor development and fostering regression if in combination of αPD-1. According to single-cell RNA sequencing (scRNA-seq), Apoe deletion was correlated with the decline of C1QC and CCR2 macrophage within tumor infiltration, and mass spectrometry results noticeably showed down-regulated the number of M2 macrophages as well. Furthermore, APOE expression in cancer patients resistant to αPD-1 treatment significantly exceeded that in the sensitive group. For this reason, APOE is likely to be targeted for modifying tumor macrophage infiltrate and augmenting checkpoint immunotherapy.

摘要

检查点免疫疗法能够释放 T 细胞来控制肿瘤,然而它却被免疫抑制性髓样细胞所破坏。载脂蛋白 E(APOE)是 LDL 受体家族成员中的一种配体,介导载脂蛋白 B 参与动脉粥样硬化脂蛋白的清除。此外,肿瘤浸润巨噬细胞可以表达 APOE。本研究报告称,与野生型相比,Apoe 小鼠对三种类型的癌发展具有更高的抗性,并且对 αPD-1(抗 PD-1)免疫疗法有更大的反应。此外,如果与 αPD-1 联合使用,利用 APOE 抑制剂(COG 133TFA,αAPOE)进行治疗能够抑制肿瘤的发展并促进其消退。根据单细胞 RNA 测序(scRNA-seq),Apoe 缺失与肿瘤浸润中 C1QC 和 CCR2 巨噬细胞的减少相关,并且质谱结果明显显示 M2 巨噬细胞的数量也减少了。此外,对αPD-1 治疗有抗性的癌症患者的 APOE 表达明显高于敏感组。因此,APOE 可能成为靶向修饰肿瘤巨噬细胞浸润和增强检查点免疫疗法的靶点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/754a/9461658/98d143d00682/ijbsv18p5230g009.jpg
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