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ADAR1 在 RNA 沉默中的拮抗和刺激作用。

Antagonistic and stimulative roles of ADAR1 in RNA silencing.

机构信息

The Wistar Institute; Philadelphia, PA USA.

出版信息

RNA Biol. 2013 Aug;10(8):1240-7. doi: 10.4161/rna.25947. Epub 2013 Jul 30.

Abstract

Adenosine deaminases acting on RNA (ADARs) are involved in RNA editing that converts adenosine residues to inosine specifically in double-stranded RNAs (dsRNA). This A-to-I RNA editing pathway and the RNA interference (RNAi) pathway seem to interact antagonistically by competing for their common dsRNA substrates. For instance, A-to-I editing of certain microRNA (miRNA) precursors by ADAR1 and ADAR2 inhibits their processing to mature miRNAs. Recent studies unexpectedly revealed the presence of a completely different type of interaction between the RNA editing mechanism and the RNAi machinery. ADAR1 forms a complex via direct protein-protein interaction with Dicer, an RNase III gene family member involved in the RNAi mechanism. ADAR1 in the Dicer complex promotes pre-miRNA cleavage by Dicer and facilitates loading of miRNA onto RNA-induced silencing complexes, giving rise to an unsuspected stimulative function of ADAR1 on miRNA processing and RNAi mechanisms. ADAR1 differentiates its functions in RNA editing and RNAi by formation of either ADAR1-ADAR1 homodimer or Dicer-ADAR1 heterodimer complexes. Expression of miRNAs is globally inhibited in ADAR1-null mouse embryos, which, in turn, alters expression of their target genes and may contribute to their embryonic lethal phenotype.

摘要

作用于 RNA 的腺苷脱氨酶 (ADARs) 参与 RNA 编辑,该编辑将腺苷残基特异性地转换为双链 RNA (dsRNA) 中的肌苷。这种 A 到 I 的 RNA 编辑途径和 RNA 干扰 (RNAi) 途径似乎通过竞争其共同的 dsRNA 底物而相互拮抗。例如,ADAR1 和 ADAR2 对某些 microRNA (miRNA) 前体的 A 到 I 编辑抑制了它们加工成熟 miRNA 的过程。最近的研究出人意料地揭示了 RNA 编辑机制与 RNAi 机制之间存在完全不同类型的相互作用。ADAR1 通过与 Dicer 的直接蛋白-蛋白相互作用形成复合物,Dicer 是一种参与 RNAi 机制的 RNase III 基因家族成员。Dicer 复合物中的 ADAR1 促进 Dicer 对 pre-miRNA 的切割,并有助于 miRNA 加载到 RNA 诱导的沉默复合物上,从而对 miRNA 加工和 RNAi 机制产生意想不到的刺激作用。ADAR1 通过形成 ADAR1-ADAR1 同源二聚体或 Dicer-ADAR1 异源二聚体复合物来区分其在 RNA 编辑和 RNAi 中的功能。ADAR1 缺失的小鼠胚胎中 miRNA 的表达被全局性抑制,这反过来又改变了它们靶基因的表达,并可能促成其胚胎致死表型。

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