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神经内分泌相关自身抗原的胸腺库:在T细胞选择中的生物学作用及药理学意义。

The thymic repertoire of neuroendocrine-related self antigens: biological role in T-cell selection and pharmacological implications.

作者信息

Geenen V, Kecha O, Brilot F, Charlet-Renard C, Martens H

机构信息

Institute of Pathology CHU-B23, Laboratory of Radioimmunology and Neuroendocrine-Immunology, University of Liège, Belgium.

出版信息

Neuroimmunomodulation. 1999 Jan-Apr;6(1-2):115-25. doi: 10.1159/000026371.

Abstract

Thymic epithelium, including nurse cells (TEC/TNC), as well as other thymic stromal cells (macrophages and dentritic cells), express a repertoire of polypeptide belonging to various neuroendocrine protein families (such as the neurophypophysial, tachykinin, neurotensin and insulin families). A hierarchy of dominance exists in the organization of the thymic repertoire of neuroendocrine precursors. Oxytocin (OT) is more expressed in the TEC/TNC than vasopressin (VP); insulin-like growth factor 2 (IGF-2) thymic expression predominates over IGF-1, and much more over (pro)insulin. Thus, OT was proposed to be the self antigen of the neurohypophysial family, and IGF-2 the self antigen precursor of the insulin family. The dual role of the thymus in T-cell life and death is recapitulated at the level of the thymic neuroendocrine protein repertoire. Indeed, thymic polypeptides behave as accessory signals involved in T-cell development and positive selection according to the cryptocrine model of signaling. Moreover, thymic neuroendocrine polypeptides are the source of self antigens presented by thymic MHC molecules to developing pre-T cells. This presentation might induce the negative selection of T cells bearing a randomly rearranged antigen receptor (TCR) oriented against neuroendocrine families. Using an animal model of autoimmune type 1 diabetes (BB rat), we have shown a defect in intrathymic expression of the self antigen of the insulin family (IGF-2) and in IGF-2-mediated T-cell education to recognize and tolerate the insulin family. Altogether these studies have enlightened the crucial role played by the thymus in the induction of the central self tolerance of neuroendocrine families. The tolerogenic properties of thymic self peptides could be used in a novel type of vaccination for the prevention of autoimmune diseases.

摘要

胸腺上皮细胞,包括哺育细胞(TEC/TNC),以及其他胸腺基质细胞(巨噬细胞和树突状细胞),表达属于各种神经内分泌蛋白家族(如神经垂体、速激肽、神经降压素和胰岛素家族)的一系列多肽。在胸腺神经内分泌前体的组织中存在优势等级。催产素(OT)在TEC/TNC中的表达比加压素(VP)更丰富;胰岛素样生长因子2(IGF-2)的胸腺表达比IGF-1占优势,且比(前)胰岛素更占优势。因此,OT被认为是神经垂体家族的自身抗原,而IGF-2是胰岛素家族的自身抗原前体。胸腺在T细胞生死中的双重作用在胸腺神经内分泌蛋白库水平上得以体现。事实上,根据信号分泌模型,胸腺多肽作为参与T细胞发育和阳性选择的辅助信号。此外,胸腺神经内分泌多肽是胸腺MHC分子呈递给发育中的前T细胞的自身抗原的来源。这种呈递可能诱导带有针对神经内分泌家族随机重排抗原受体(TCR)的T细胞的阴性选择。使用自身免疫性1型糖尿病动物模型(BB大鼠),我们已经证明胰岛素家族自身抗原(IGF-2)的胸腺内表达存在缺陷,以及IGF-2介导的T细胞识别和耐受胰岛素家族的教育存在缺陷。总之,这些研究揭示了胸腺在诱导神经内分泌家族中枢自身耐受中所起的关键作用。胸腺自身肽的致耐受性特性可用于一种新型疫苗接种以预防自身免疫性疾病。

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