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RNA Editing ADAR1 and the Innate Immune Response

机译:RNA编辑ADAR1和先天免疫反应

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摘要

RNA editing, particularly A-to-I RNA editing, has been shown to play an essential role in mammalian embryonic development and tissue homeostasis, and is implicated in the pathogenesis of many diseases including skin pigmentation disorder, autoimmune and inflammatory tissue injury, neuron degeneration, and various malignancies. A-to-I RNA editing is carried out by a small group of enzymes, the adenosine deaminase acting on RNAs (ADARs). Only three members of this protein family, ADAR1–3, exist in mammalian cells. ADAR3 is a catalytically null enzyme and the most significant function of ADAR2 was found to be in editing on the neuron receptor GluR-B mRNA. ADAR1, however, has been shown to play more significant roles in biological and pathological conditions. Although there remains much that is not known about how ADAR1 regulates cellular function, recent findings point to regulation of the innate immune response as an important function of ADAR1. Without appropriate RNA editing by ADAR1, endogenous RNA transcripts stimulate cytosolic RNA sensing receptors and therefore activate the IFN-inducing signaling pathways. Overactivation of innate immune pathways can lead to tissue injury and dysfunction. However, obvious gaps in our knowledge persist as to how ADAR1 regulates innate immune responses through RNA editing. Here, we review critical findings from ADAR1 mechanistic studies focusing on its regulatory function in innate immune responses and identify some of the important unanswered questions in the field.
机译:RNA编辑,尤其是从A到I的RNA编辑,已显示在哺乳动物胚胎发育和组织体内平衡中起着至关重要的作用,并且与许多疾病的发病机理有关,包括皮肤色素沉着症,自身免疫和炎性组织损伤,神经元变性,以及各种恶性肿瘤。 A对I RNA编辑是通过一小组酶(作用于RNA(ADAR)的腺苷脱氨酶)进行的。该蛋白质家族中只有三个成员ADAR1-3存在于哺乳动物细胞中。 ADAR3是一种无催化活性的酶,发现ADAR2的最重要功能是在神经元受体GluR-B mRNA的编辑中。然而,已经显示出ADAR1在生物学和病理学状况中起着更重要的作用。尽管关于ADAR1如何调节细胞功能仍有许多未知,但最近的发现表明,先天免疫应答的调节是ADAR1的重要功能。如果没有通过ADAR1进行适当的RNA编辑,内源性RNA转录物会刺激胞质RNA感应受体,从而激活IFN诱导的信号通路。先天免疫途径的过度激活会导致组织损伤和功能障碍。但是,关于ADAR1如何通过RNA编辑调节先天免疫应答的知识仍然存在明显的差距。在这里,我们回顾了ADAR1机制研究的关键发现,重点是其在先天免疫应答中的调节功能,并确定了该领域中一些重要的未解决问题。

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