How RNA editing keeps an I on physiology

阿达尔 生物 核糖核酸 RNA编辑 碱基对 翻译(生物学) 遗传学 非编码RNA 核糖体 计算生物学 基因 细胞生物学 信使核糖核酸
作者
Marion Goldeck,Aiswarya Gopal,Michael F. Jantsch,Hamid R. Mansouri,Vinod Rajendra,Cornelia Vesely
出处
期刊:American Journal of Physiology-cell Physiology [American Physical Society]
卷期号:323 (5): C1496-C1511 被引量:6
标识
DOI:10.1152/ajpcell.00191.2022
摘要

Adenosine deaminases acting on RNAs convert adenosines (A) to inosines (I) in structured or double-stranded RNAs. In mammals, this process is widespread. In the human transcriptome, more than a million different sites have been identified that undergo an ADAR-mediated A-to-I exchange Inosines have an altered base pairing potential due to the missing amino group when compared to the original adenosine. Consequently, inosines prefer to base pair with cytosines but can also base pair with uracil or adenine. This altered base pairing potential not only affects protein decoding at the ribosome but also influences the folding of RNAs and the proteins that can associate with it. Consequently, an A to I exchange can also affect RNA processing and turnover (Nishikura K. Annu Rev Biochem 79: 321-349, 2010; Brümmer A, Yang Y, Chan TW, Xiao X. Nat Commun 8: 1255, 2017). All of these events will interfere with gene expression and therefore, can also affect cellular and organismic physiology. As double-stranded RNAs are a hallmark of viral pathogens RNA-editing not only affects RNA-processing, coding, and gene expression but also controls the antiviral response to double-stranded RNAs. Most interestingly, recent advances in our understanding of ADAR enzymes reveal multiple layers of regulation by which ADARs can control antiviral programs. In this review, we focus on the recoding of mRNAs where the altered translation products lead to physiological changes. We also address recent advances in our understanding of the multiple layers of antiviral responses and innate immune modulations mediated by ADAR1.

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