Tumor-associated protein ligands recognized by human γδ T cell receptor and their implications in cancer therapy

Chang Liu, Yi Xu, Jianmin Zhang, Wei He
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Abstract

In recent years, immunologists have been working to utilize the functional mechanism of the immune system to research new tumor treatment methods and achieved a major breakthrough in 2013, which was listed as one of the top 10 scientific breakthroughs of 2013 by Science magazine (see “Cancer immunotherapy”. Science. 2013;342:1417. doi: 10.1126/science.1249481). Currently, two main methods are used in clinical tumor immunotherapy: immune checkpoint inhibitors and chimeric antigen receptor (CAR) T cells. Clinical responses to checkpoint inhibitors rely on blockade of the target neoantigens expressed on the surfaces of tumor cells, which can inhibit T cell activity and prevent the T cell immune response; therefore, the therapeutic effect is limited by the tumor antigen expression level. While CAR-T cell therapy can partly enhance neoantigen recognition of T cells, problems remain in the current treatment for solid tumors, such as restricted transport of adoptively transferred cells to the tumor site and off-targets. Immunologists have therefore turned their attention to γδ T cells, which are not restricted by the major histocompatibility complex (MHC) for neoantigen recognition and are able to initiate a rapid immune response at an early stage. However, due to the lack of an understanding of the antigens that γδ T cells recognize, the role of γδ T cells in tumorigenesis and tumor development is not clearly understood. In the past few years, extensive data identifying antigen ligands recognized by γδ T cells have been obtained, mainly focusing on bisphosphonates and small-molecule polypeptides, but few studies have focused on protein ligands recognized by γδ T cells. In this paper, it is reviewed and analyzed that the tumor-associated protein ligands of γδ T cells that have been discovered thus far, hoping to provide new ideas for the comprehensive application of γδ T cells in tumor immunotherapy.
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人γδT细胞受体识别的肿瘤相关蛋白配体及其在癌症治疗中的意义
近年来,免疫学家一直致力于利用免疫系统的功能机制来研究新的肿瘤治疗方法,并于2013年取得了重大突破,被《科学》杂志列为2013年十大科学突破之一(见“癌症免疫治疗”)。科学。2013;342:1417。doi: 10.1126 / science.1249481)。目前,临床肿瘤免疫治疗主要采用两种方法:免疫检查点抑制剂和CAR - T细胞。检查点抑制剂的临床应答依赖于阻断肿瘤细胞表面表达的靶新抗原,从而抑制T细胞活性,阻止T细胞免疫应答;因此,治疗效果受到肿瘤抗原表达水平的限制。虽然CAR-T细胞疗法可以在一定程度上增强T细胞对新抗原的识别,但目前对实体瘤的治疗仍然存在一些问题,例如过继转移细胞到肿瘤部位的运输受限和脱靶。因此,免疫学家将注意力转向了γδ T细胞,它不受主要组织相容性复合体(MHC)对新抗原识别的限制,能够在早期阶段启动快速的免疫反应。然而,由于缺乏对γδ T细胞识别的抗原的了解,γδ T细胞在肿瘤发生和肿瘤发展中的作用尚不清楚。近年来,关于γδ T细胞识别抗原配体的研究数据较多,主要集中在双膦酸盐类和小分子多肽类,而关于γδ T细胞识别蛋白质配体的研究较少。本文对目前已发现的γδ T细胞肿瘤相关蛋白配体进行综述和分析,希望为γδ T细胞在肿瘤免疫治疗中的综合应用提供新的思路。
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