Ly6E on tumor cells impairs anti-tumor T-cell responses: a novel mechanism of tumor-induced immune exclusion.

IF 4.6 2区 医学 Q2 IMMUNOLOGY Cancer Immunology, Immunotherapy Pub Date : 2024-11-02 DOI:10.1007/s00262-024-03851-x
Lan Hailin, Chen Yiting, Wu Yue, Li Lijun, Zhang Renlu, Chen Yunhan, Zhu Yanyang, Zhang Qiuyu
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Abstract

Background: Lymphocyte antigen 6 complex, locus E (Ly6E) has been initially demonstrated to involve in T cell activity and impair viral infectivity. Recently, high expression levels of Ly6E have been reported in tumor microenvironment (TME) of various types of cancers. However, the immunoregulatory mechanism of Ly6E manipulating TME remains unknown.

Methods: TCGA database and Kaplan-Meier plotter database were used to evaluate the correlation between Ly6E expression levels and cancer patient survival. After analyzing Ly6E expression levels in human breast cancer tissues and tumor cell lines, we generated Ly6E knockout (KO) and overexpression (OE) mouse cell lines. Cell proliferation ability in vitro and the ability of growth and metastasis in mouse tumor models were compared between KO/OE and wild-type tumor cells. On day 7 after tumor implantation, tumor tissues were separated for flow cytometric assay, bulk RNA sequencing and single-cell RNA sequencing (ScRNA-seq). The role of Ly6E-expressing tumor cell on macrophage was analyzed in vitro.

Results: Our result surprisingly found that high Ly6E expression levels were associated with CD8+ T cell exclusion in tumor tissues and resistance to immunotherapy. Our data showed that knockout of Ly6E in tumor cells prompts tumor regression and inhibits tumor metastases, and Ly6E-OE tumor cells vice versa. The enhanced anti-tumor effect of Ly6E knockout in tumor cells was dependent on T cell response and formed long-lasting memory. The increase in the CD8+ T-cell infiltration into the tumor islet of Ly6E-KO tumors confirmed the role of Ly6E on T cell exclusion. ScRNA-seq analysis showed that M2 macrophages are particularly abundant in the Ly6E-expressing tumor tissues, especially M2-4 macrophage cluster identified by high levels of Arg-1, indicates that Ly6E-expressing tumor cells might restrict T cell infiltration via M2 macrophages. Moreover, in vitro assay showed that cell culture media derived from Ly6E-positive tumor cells promoted macrophage migration and M2 polarization.

Conclusion: Our study illuminated that Ly6E-expressing tumor cells facilitated the accumulation of M2 macrophages in TME, which contributes to CD8+ T cell exclusion and provides new insights for improving efficacy of cancer immunotherapy.

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肿瘤细胞上的 Ly6E 会损害抗肿瘤 T 细胞反应:肿瘤诱导免疫排斥的新机制。
背景:淋巴细胞抗原 6 复合物,位点 E(Ly6E)已被初步证实参与 T 细胞活性并损害病毒的感染性。最近,有报道称 Ly6E 在各种类型癌症的肿瘤微环境(TME)中高水平表达。然而,Ly6E操纵TME的免疫调节机制仍然未知:方法:利用 TCGA 数据库和 Kaplan-Meier plotter 数据库评估 Ly6E 表达水平与癌症患者生存期的相关性。在分析了人类乳腺癌组织和肿瘤细胞系中的 Ly6E 表达水平后,我们生成了 Ly6E 基因敲除(KO)和过表达(OE)小鼠细胞系。比较了 KO/OE 和野生型肿瘤细胞在体外的增殖能力以及在小鼠肿瘤模型中的生长和转移能力。在肿瘤植入后第7天,分离肿瘤组织进行流式细胞分析、大量RNA测序和单细胞RNA测序(ScRNA-seq)。在体外分析了表达 Ly6E 的肿瘤细胞对巨噬细胞的作用:结果:我们惊讶地发现,Ly6E的高表达水平与肿瘤组织中CD8+ T细胞的排斥和对免疫疗法的抵抗有关。我们的数据显示,敲除肿瘤细胞中的 Ly6E 可促使肿瘤消退并抑制肿瘤转移,反之亦然。敲除肿瘤细胞中的 Ly6E 所增强的抗肿瘤作用依赖于 T 细胞反应并形成持久记忆。Ly6E-KO肿瘤的CD8+ T细胞对肿瘤胰岛浸润的增加证实了Ly6E对T细胞排斥的作用。ScRNA-seq分析表明,M2巨噬细胞在Ly6E表达的肿瘤组织中特别丰富,尤其是M2-4巨噬细胞集群,其Arg-1水平很高,这表明Ly6E表达的肿瘤细胞可能通过M2巨噬细胞限制了T细胞的浸润。此外,体外实验表明,来自Ly6E阳性肿瘤细胞的细胞培养基可促进巨噬细胞迁移和M2极化:我们的研究表明,Ly6E表达的肿瘤细胞促进了M2巨噬细胞在TME中的聚集,这有助于CD8+ T细胞的排斥,并为提高癌症免疫疗法的疗效提供了新的见解。
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来源期刊
CiteScore
10.50
自引率
1.70%
发文量
207
审稿时长
1 months
期刊介绍: Cancer Immunology, Immunotherapy has the basic aim of keeping readers informed of the latest research results in the fields of oncology and immunology. As knowledge expands, the scope of the journal has broadened to include more of the progress being made in the areas of biology concerned with biological response modifiers. This helps keep readers up to date on the latest advances in our understanding of tumor-host interactions. The journal publishes short editorials including "position papers," general reviews, original articles, and short communications, providing a forum for the most current experimental and clinical advances in tumor immunology.
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