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Neonatal tolerance revisited: a perinatal window for Aire control of autoimmunity

机译:再谈新生儿耐受性:艾尔控制自身免疫的围产期窗口

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摘要

There has long been conceptual and experimental support for, but also challenges to, the notion that the initial period of the immune system's development is particularly important for the establishment of tolerance to self. The display of self-antigens by thymic epithelial cells is key to inducing tolerance in the T lymphocyte compartment, a process enhanced by the Aire transcription factor. Using a doxycycline-regulated transgene to target Aire expression to the thymic epithelium, complementing the Aire knockout in a temporally controlled manner, we find that Aire is essential in the perinatal period to prevent the multiorgan autoimmunity that is typical of Aire deficiency. Surprisingly, Aire could be shut down soon thereafter and remain off for long periods, with few deleterious consequences. The lymphopenic state present in neonates was a factor in this dichotomy because inducing lymphopenia during Aire turnoff in adults recreated the disease, which, conversely, could be ameliorated by supplementing neonates with adult lymphocytes. In short, Aire expression during the perinatal period is both necessary and sufficient to induce long-lasting tolerance and avoid autoimmunity. Aire-controlled mechanisms of central tolerance are largely dispensable in the adult, as a previously tolerized T cell pool can buffer newly generated autoreactive T cells that might emerge.
机译:长期以来,对于免疫系统发育初期对于建立自我耐受性特别重要的观念一直存在观念和实验上的支持,但也面临挑战。胸腺上皮细胞显示自身抗原是诱导T淋巴细胞区室的耐受性的关键,这一过程由Aire转录因子增强。使用强力霉素调节的转基因将Aire表达靶向胸腺上皮,以时间控制的方式补充Aire基因敲除,我们发现Aire在围产期至关重要,可预防Aire缺乏典型的多器官自身免疫。出人意料的是,此后不久,艾尔(Aire)可能会关闭,并长时间保持关闭状态,几乎没有有害后果。新生儿中存在的淋巴细胞减少状态是这种二分法的一个因素,因为在成年人的Aire关机期间诱导淋巴细胞减少会重现该病,反之,可以通过向新生儿补充成人淋巴细胞来缓解这种疾病。简而言之,围产期Aire表达对于诱导持久耐受和避免自身免疫是必要且充分的。在成年人中,艾里控制的中央耐受机制在很大程度上是必需的,因为以前耐受的T细胞库可以缓冲可能出现的新生成的自身反应性T细胞。

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