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Dendritic cell maturation: functional specialization through signaling specificity and transcriptional programming

机译:树突状细胞成熟:通过信号传导特异性和转录编程实现功能专一

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摘要

Dendritic cells (DC) are key regulators of both protective immune responses and tolerance to self-antigens. Soon after their discovery in lymphoid tissues by Steinman and Cohn, as cells with the unique ability to prime naïve antigen-specific T cells, it was realized that DC can exist in at least two distinctive states characterized by morphological, phenotypic and functional changes—this led to the description of DC maturation. It is now well appreciated that there are several subsets of DC in both lymphoid and non-lymphoid tissues of mammals, and these cells show remarkable functional specialization and specificity in their roles in tolerance and immunity. This review will focus on the specific characteristics of DC subsets and how their functional specialization may be regulated by distinctive gene expression programs and signaling responses in both steady-state and in the context of inflammation. In particular, we will highlight the common and distinctive genes and signaling pathways that are associated with the functional maturation of DC subsets.
机译:树突状细胞(DC)是保护性免疫反应和对自身抗原耐受性的关键调节剂。 Steinman和Cohn在淋巴组织中发现它们后,很快就发现它们具有引发初生抗原特异性T细胞的独特能力,很快就意识到DC可以以形态,表型和功能变化为特征的至少两种不同状态存在。导致了对DC成熟的描述。现在众所周知,在哺乳动物的淋巴组织和非淋巴组织中都存在DC的几个子集,并且这些细胞在耐受性和免疫性中的作用显示出显着的功能专一性和特异性。这篇综述将集中在DC亚群的具体特征上,以及它们的功能专一性如何通过独特的基因表达程序和发信号的稳态和炎症反应来调节。特别是,我们将重点介绍与DC子集功能成熟相关的共同和独特的基因和信号通路。

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