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HLA-C 在母体-胎儿界面的耐受和免疫中的双重作用。

The Dual Role of HLA-C in Tolerance and Immunity at the Maternal-Fetal Interface.

机构信息

Department of Stem Cell and Regenerative Biology, Harvard University, Cambridge, MA, United States.

Department of Surgery, Beth Israel Deaconess Medical Center, Boston, MA, United States.

出版信息

Front Immunol. 2019 Dec 9;10:2730. doi: 10.3389/fimmu.2019.02730. eCollection 2019.

Abstract

To establish a healthy pregnancy, maternal immune cells must tolerate fetal allo-antigens and remain competent to respond to infections both systemically and in placental tissues. Extravillous trophoblasts (EVT) are the most invasive cells of extra-embryonic origin to invade uterine tissues and express polymorphic Human Leucocyte Antigen-C (HLA-C) of both maternal and paternal origin. Thus, HLA-C is a key molecule that can elicit allogeneic immune responses by maternal T and NK cells and for which maternal-fetal immune tolerance needs to be established. HLA-C is also the only classical MHC molecule expressed by EVT that can present a wide variety of peptides to maternal memory T cells and establish protective immunity. The expression of paternal HLA-C by EVT provides a target for maternal NK and T cells, whereas HLA-C expression levels may influence how this response is shaped. This dual function of HLA-C requires tight transcriptional regulation of its expression to balance induction of tolerance and immunity. Here, we critically review new insights into: (i) the mechanisms controlling expression of HLA-C by EVT, (ii) the mechanisms by which decidual NK cells, effector T cells and regulatory T cells recognize HLA-C allo-antigens, and (iii) immune recognition of pathogen derived antigens in context of HLA-C.

摘要

为了建立健康的妊娠,母体免疫细胞必须耐受胎儿同种异体抗原,并保持对全身和胎盘组织感染的有效反应能力。绒毛外滋养细胞(EVT)是最具侵袭性的胚胎外起源细胞,可侵入子宫组织,并表达母体和父体来源的多态性人类白细胞抗原-C(HLA-C)。因此,HLA-C 是一种关键分子,可以通过母体 T 和 NK 细胞引发同种异体免疫反应,而母体-胎儿免疫耐受需要建立。HLA-C 也是 EVT 表达的唯一经典 MHC 分子,可向母体记忆 T 细胞呈递多种肽段,并建立保护性免疫。EVT 表达的父系 HLA-C 为母体 NK 和 T 细胞提供了一个靶标,而 HLA-C 的表达水平可能影响这种反应的形成方式。HLA-C 的这种双重功能需要其表达的严格转录调控,以平衡诱导的耐受性和免疫性。在这里,我们批判性地回顾了有关以下方面的新见解:(i)控制 EVT 表达 HLA-C 的机制,(ii)蜕膜 NK 细胞、效应 T 细胞和调节 T 细胞识别 HLA-C 同种异体抗原的机制,以及(iii)在 HLA-C 背景下对病原体衍生抗原的免疫识别。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a804/6913657/3ae153f89f51/fimmu-10-02730-g0001.jpg

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