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The Epitranscriptome and Innate Immunity

机译:转录组和先天免疫

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摘要

Our knowledge of the variety and abundances of RNA base modifications is rapidly increasing. Modified bases have critical roles in tRNAs, rRNAs, translation, splicing, RNA interference, and other RNA processes, and are now increasingly detected in all types of transcripts. Can new biological principles associated with this diversity of RNA modifications, particularly in mRNAs and long non-coding RNAs, be identified? This review will explore this question by focusing primarily on adenosine to inosine (A-to-I) RNA editing by the adenine deaminase acting on RNA (ADAR) enzymes that have been intensively studied for the past 20 years and have a wide range of effects. Over 100 million adenosine to inosine editing sites have been identified in the human transcriptome, mostly in embedded Alu sequences that form potentially innate immune-stimulating dsRNA hairpins in transcripts. Recent research has demonstrated that inosine in the epitranscriptome and ADAR1 protein establish innate immune tolerance for host dsRNA formed by endogenous sequences. Innate immune sensors that detect viral nucleic acids are among the readers of epitranscriptome RNA modifications, though this does preclude a wide range of other modification effects.
机译:我们对RNA碱基修饰的多样性和丰富性的了解正在迅速增加。修饰的碱基在tRNA,rRNA,翻译,剪接,RNA干扰和其他RNA过程中起着至关重要的作用,并且现在在所有类型的转录物中越来越多地被检测到。是否可以确定与这种RNA修饰多样性相关的新生物学原理,尤其是在mRNA和长的非编码RNA中?这篇综述将主要通过腺苷脱氨酶作用于RNA(ADAR)酶的腺苷到肌苷(A-to-I)RNA编辑来探讨这个问题,该酶在过去20年中已被广泛研究并具有广泛的作用。在人类转录组中已鉴定出超过1亿个腺苷到肌苷的编辑位点,主要是在嵌入的Alu序列中,这些序列在转录物中形成了潜在的先天性免疫刺激dsRNA发夹。最近的研究表明,转录组中的肌苷和ADAR1蛋白对由内源序列形成的宿主dsRNA建立先天免疫耐受。能够检测病毒核酸的先天免疫传感器属于转录组RNA修饰的读者,尽管这确实排除了其他多种修饰作用。

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