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胸腺皮质上皮细胞可在体内呈递自身抗原。

Thymic cortical epithelial cells can present self-antigens in vivo.

作者信息

Lorenz R G, Allen P M

机构信息

Department of Pathology, Washington University School of Medicine, St Louis, Missouri 63110.

出版信息

Nature. 1989 Feb 9;337(6207):560-2. doi: 10.1038/337560a0.

Abstract

Antigens present during neonatal life are recognized as self and individuals are tolerant to these antigens. In normal individuals T cells are tolerant to most self proteins but we still know little of the mechanism(s) by which tolerance is established. A requisite part of the current negative selection model of self tolerance is the expression of self proteins complexed with major histocompatibility complex molecules in the thymus. As MHC proteins bind antigens and present them to the receptor on the antigen-specific T cell, then for tolerance to self to occur, it is possible that each self protein must be processed and presented by an MHC molecule. As a result of the development of a unique T-cell hybrid reactive to the self protein murine haemoglobin, we have shown that in normal animals this self protein is continuously processed and potentially presented in an MHC-restricted manner. Here we show that self haemoglobin is being processed and presented by thymic antigen-presenting cells as early as gestational day 14. We also demonstrate that three types of thymic stromal cells, namely macrophages, dendritic cells and cortical epithelial cells, can present the haemoglobin self antigen in vivo. This surprising presentation of a self antigen by thymic cortical epithelial cells implies that they could be involved in T-cell development and negative selection.

摘要

新生儿期存在的抗原被识别为自身抗原,个体对这些抗原具有耐受性。在正常个体中,T细胞对大多数自身蛋白质具有耐受性,但我们对建立耐受性的机制仍知之甚少。当前自身耐受性阴性选择模型的一个必要部分是与主要组织相容性复合体分子复合的自身蛋白质在胸腺中的表达。由于MHC蛋白结合抗原并将其呈递给抗原特异性T细胞上的受体,那么为了发生对自身的耐受性,每个自身蛋白质必须由MHC分子进行加工和呈递。由于开发出了一种对自身蛋白质小鼠血红蛋白有反应的独特T细胞杂交体,我们已经表明,在正常动物中,这种自身蛋白质会持续被加工,并可能以MHC限制的方式呈递。在这里我们表明,早在妊娠第14天,自身血红蛋白就被胸腺抗原呈递细胞加工并呈递。我们还证明,三种类型的胸腺基质细胞,即巨噬细胞、树突状细胞和皮质上皮细胞,能够在体内呈递血红蛋白自身抗原。胸腺皮质上皮细胞对自身抗原的这种惊人呈递意味着它们可能参与T细胞的发育和阴性选择。

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