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胸腺中的抗原呈递细胞可对识别循环自身抗原的MHC II类限制性T细胞进行阴性选择。

Antigen-presenting cells in the thymus that can negatively select MHC class II-restricted T cells recognizing a circulating self antigen.

作者信息

Volkmann A, Zal T, Stockinger B

机构信息

Division of Molecular Immunology, National Institute for Medical Research, London, United Kingdom.

出版信息

J Immunol. 1997 Jan 15;158(2):693-706.

PMID:8992985
Abstract

We investigated Ag presentation of an extracellular self Ag (C5), which only reaches the thymus via the blood circulation, for negative selection of MHC class II-restricted, C5-specific T cells. Thymic APC were introduced into fetal thymic reaggregation culture with thymocytes from C5-specific TCR transgenic mice to follow the development of C5-specific T cells in the presence or the absence of self Ag presented by various APC. To mimic the physiologic distribution of C5 peptide/MHC class II complexes on thymic APC as closely as possible, they were isolated from thymi of C5+ mice, so that the amount of C5 peptide bound to MHC class II on their surface would reflect the amount of self Ag they have access to and process normally in vivo. This circumvented the problems related to artificially high doses of Ag or peptide in vivo or in vitro, that might obscure physiologic differences such as the capacity to internalize and process Ag. The results show that not only thymic dendritic cells, but also cortical and medullary epithelial cells were able to induce negative selection of C5-specific thymocytes with similar efficiency. In contrast, thymic macrophages were unable to influence the development of C5-specific T cells. Their failure to present exogenous self Ag for negative selection suggests that macrophages concentrate on their primary function in the thymus, the disposal of dying thymocytes.

摘要

我们研究了细胞外自身抗原(C5)的抗原提呈,该抗原仅通过血液循环到达胸腺,用于对MHC II类限制性、C5特异性T细胞进行阴性选择。将胸腺抗原呈递细胞(APC)与来自C5特异性TCR转基因小鼠的胸腺细胞一起引入胎儿胸腺重聚集培养中,以追踪在存在或不存在各种APC提呈的自身抗原的情况下C5特异性T细胞的发育情况。为了尽可能模拟C5肽/MHC II类复合物在胸腺APC上的生理分布,从C5+小鼠的胸腺中分离出这些细胞,这样它们表面与MHC II类结合的C5肽的量就会反映出它们在体内正常接触和加工的自身抗原的量。这避免了体内或体外人为高剂量抗原或肽相关的问题,这些问题可能会掩盖诸如内化和加工抗原能力等生理差异。结果表明,不仅胸腺树突状细胞,而且皮质和髓质上皮细胞都能够以相似的效率诱导C5特异性胸腺细胞的阴性选择。相比之下,胸腺巨噬细胞无法影响C5特异性T细胞的发育。它们未能提呈外源性自身抗原进行阴性选择,这表明巨噬细胞专注于其在胸腺中的主要功能,即处理死亡的胸腺细胞。

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