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HLA-DO and Its Role in MHC Class II Antigen Presentation

机译:HLA-DO及其在MHC II类抗原呈递中的作用

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摘要

Helper T cells are stimulated to fight infections or diseases upon recognition of peptides from antigens that are processed and presented by the proteins of Major Histocompatibility Complex (MHC) Class II molecules. Degradation of a full protein into small peptide fragments is a lengthy process consisting of many steps and chaperones. Malfunctions during any step of antigen processing could lead to the development of self-reactive T cells or defective immune response to pathogens. Although much has been accomplished regarding how antigens are processed and presented to T cells, many questions still remain unanswered, preventing the design of therapeutics for direct intervention with antigen processing. Here, we review published work on the discovery and function of a MHC class II molecular chaperone, HLA-DO, in human, and its mouse analog H2-O, herein called DO. While DO was originally discovered decades ago, elucidating its function has proven challenging. DO was discovered in association with another chaperone HLA-DM (DM) but unlike DM, its distribution is more tissue specific, and its function more subtle.
机译:识别来自主要组织相容性复合体(MHC)II类分子的蛋白质加工并呈递的抗原肽后,刺激辅助T细胞抵抗感染或疾病。完整蛋白质降解为小肽片段是一个漫长的过程,包括许多步骤和分子伴侣。抗原加工的任何步骤中的功能异常都可能导致自身反应性T细胞的发育或对病原体的免疫反应不足。尽管在如何处理抗原以及将抗原呈递给T细胞方面已经取得了很多成就,但许多问题仍未解决,从而阻碍了直接干预抗原处理的治疗药物的设计。在这里,我们回顾了有关人类中MHC II类分子伴侣HLA-DO及其小鼠类似物H2-O(在此称为DO)的发现和功能的已发表工作。尽管DO最初是在几十年前发现的,但阐明其功能却被证明具有挑战性。 DO与另一种伴侣HLA-DM(DM)结合被发现,但与DM不同,DO的分布更具组织特异性,其功能更微妙。

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