首页> 美国卫生研究院文献>Nucleic Acids Research >Human MARF1 is an endoribonuclease that interacts with the DCP1:2 decapping complex and degrades target mRNAs
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Human MARF1 is an endoribonuclease that interacts with the DCP1:2 decapping complex and degrades target mRNAs

机译:人MARF1是一种内切核糖核酸酶可与DCP1:2脱盖复合物相互作用并降解目标mRNA

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摘要

Meiosis arrest female 1 (MARF1) is a cytoplasmic RNA binding protein that is essential for meiotic progression of mouse oocytes, in part by limiting retrotransposon expression. MARF1 is also expressed in somatic cells and tissues; however, its mechanism of action has yet to be investigated. Human MARF1 contains a NYN-like domain, two RRMs and eight LOTUS domains. Here we provide evidence that MARF1 post-transcriptionally silences targeted mRNAs. MARF1 physically interacts with the DCP1:DCP2 mRNA decapping complex but not with deadenylation machineries. Importantly, we provide a 1.7 Å resolution crystal structure of the human MARF1 NYN domain, which we demonstrate is a bona fide endoribonuclease, the activity of which is essential for the repression of MARF1-targeted mRNAs. Thus, MARF1 post-transcriptionally represses gene expression by serving as both an endoribonuclease and as a platform that recruits the DCP1:DCP2 decapping complex to targeted mRNAs.
机译:减数分裂雌性1(MARF1)是一种细胞质RNA结合蛋白,对小鼠卵母细胞的减数分裂进程至关重要,部分是通过限制逆转录转座子的表达。 MARF1在体细胞和组织中也有表达。然而,其作用机理尚待研究。人MARF1包含一个类似NYN的域,两个RRM和八个LOTUS域。在这里,我们提供了MARF1转录后使靶向mRNA沉默的证据。 MARF1在物理上与DCP1:DCP2 mRNA脱盖复合物相互作用,但与去烯基化机制不相互作用。重要的是,我们提供了人类MARF1 NYN域的1.7Å分辨率晶体结构,我们证明了它是一种真正的内切核糖核酸酶,其活性对于抑制MARF1靶向的mRNA是必不可少的。因此,MARF1通过充当内切核糖核酸酶和将DCP1:DCP2解壳复合物募集到目标mRNA的平台,在转录后抑制基因表达。

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