人白细胞抗原G能否被广泛接受为癌症临床的生物标志物?

K. Yie, S. Yie
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摘要

人白细胞抗原G (Human Leukocyte Antigen G, HLA-G)是一种非经典的HLA I类分子,首次在胚胎植入bbb的生殖免疫调控中被发现。由于HLA-G具有免疫抑制功能,因此一直认为HLA-G可能在肿瘤免疫逃逸机制中发挥作用。30年前,Paul等人首次报道了在黑色素瘤病变中特异性观察到HLA-G的表达。从那时起,来自30多种不同类型肿瘤的数千个样本的大量后续研究表明,HLA-G在癌症中的表达与免疫抑制微环境、肿瘤晚期、不良治疗反应和预后bbb高度相关。因此,HLA-G被推荐为一种新的生物标志物,用于人类癌症的诊断、预后和肿瘤免疫逃逸。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Can human leukocyte antigen G be widely accepted as a biomarker in cancer clinical practice?
Human Leukocyte Antigen G (HLA-G) is a non-classical HLA class I molecule that was first explored in reproductive immune regulation for fetal implantations [1]. Because HLA-G has immune suppressive functions, it has been assumed that HLA-G could play a role in tumor immune escape mechanisms. Thirty years ago, Paul et al. [2] first reported that HLA-G expression was specifically observed in melanoma lesions. Since then, numerous subsequent studies with thousands of samples from more than thirty different types of tumors have demonstrated that HLA-G expression in cancers is highly related to immune suppressive microenvironments, advanced tumor stages, and poor therapeutic responses and prognosis [3]. Accordingly, HLA-G has been recommended to be a novel biomarker for the diagnosis, prognosis, and tumor immune escape of human cancers.
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