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胸腺细胞忽视性死亡:吞噬性巨噬细胞的作用。

Thymocyte death by neglect: contribution of engulfing macrophages.

机构信息

Department of Biochemistry and Molecular Biology, Apoptosis and Genomics Research Group of the Hungarian Academy of Sciences, Research Center of Molecular Medicine, University of Debrecen, Debrecen, Hungary.

出版信息

Eur J Immunol. 2012 Jul;42(7):1662-7. doi: 10.1002/eji.201142338.

Abstract

The thymus provides the microenvironment in which thymocytes develop into mature T cells, and interactions with thymic stromal cells are thought to provide the necessary signals for thymocyte maturation. Recognition of self-MHC by T cells is a basic requirement for mature T-cell functions, and those thymocytes that do not recognize the peptide-loaded self-MHC molecules found in the thymus, and therefore lack a TCR signal, undergo a default death pathway named "death by neglect" in the thymic cortex. In the absence of this TCR signaling, it has been suggested that binding of glucocorticoids to - or the ligation of certain cell surface molecules, such as CD8, CD24, CD45, or CD99 on - these neglected thymocytes will induce them to enter the apoptotic program. Apoptotic thymocytes are cleared by the surrounding macrophages and, as a consequence, these macrophages are known to release various molecules, such as adenosine, retinoids, TGF-β, ATP, and carbon monoxide. Interestingly, all these molecules have been described to induce or promote apoptosis in thymocytes in the absence of TCR signaling. Here, we propose that thymic macrophages, because they continually engulf apoptotic cells, might constantly provide these cell death-inducing signals, and thus contribute to the formation of a thymic milieu that ensures the effective induction of "death by neglect".

摘要

胸腺为胸腺细胞发育为成熟 T 细胞提供了微环境,并且与胸腺基质细胞的相互作用被认为提供了胸腺细胞成熟所需的信号。T 细胞对自身 MHC 的识别是成熟 T 细胞功能的基本要求,那些不能识别胸腺中发现的负载肽的自身 MHC 分子的胸腺细胞,因此缺乏 TCR 信号,会经历一种在胸腺皮质中被称为“忽视性死亡”的默认死亡途径。在缺乏这种 TCR 信号的情况下,有人提出,糖皮质激素与这些被忽视的胸腺细胞上的某些细胞表面分子(如 CD8、CD24、CD45 或 CD99)的结合或连接,将诱导它们进入凋亡程序。凋亡的胸腺细胞被周围的巨噬细胞清除,因此这些巨噬细胞被认为会释放各种分子,如腺苷、类视黄醇、TGF-β、ATP 和一氧化碳。有趣的是,所有这些分子都被描述为在缺乏 TCR 信号的情况下诱导或促进胸腺细胞凋亡。在这里,我们提出胸腺巨噬细胞,因为它们不断吞噬凋亡细胞,可能会不断提供这些诱导细胞死亡的信号,从而有助于形成一个确保有效诱导“忽视性死亡”的胸腺环境。

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