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microRNAs associated with the different human Argonaute proteins

机译:与不同人类Argonaute蛋白相关的microRNA

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MicroRNAs (miRNAs) are small noncoding RNAs that function in literally all cellular processes. miRNAs interact with Argonaute (Ago) proteins and guide them to specific target sites located in the 3′-untranslated region (3′-UTR) of target mRNAs leading to translational repression and deadenylation-induced mRNA degradation. Most miRNAs are processed from hairpin-structured precursors by the consecutive action of the RNase III enzymes Drosha and Dicer. However, processing of miR-451 is Dicer independent and cleavage is mediated by the endonuclease Ago2. Here we have characterized miR-451 sequence and structure requirements for processing as well as sorting of miRNAs into different Ago proteins. Pre-miR-451 appears to be optimized for Ago2 cleavage and changes result in reduced processing. In addition, we show that the mature miR-451 only associates with Ago2 suggesting that mature miRNAs are not exchanged between different members of the Ago protein family. Based on cloning and deep sequencing of endogenous miRNAs associated with Ago1–3, we do not find evidence for miRNA sorting in human cells. However, Ago identity appears to influence the length of some miRNAs, while others remain unaffected.
机译:微小RNA(miRNA)是小的非编码RNA,实际上可以在所有细胞过程中起作用。 miRNA与Argonaute(Ago)蛋白相互作用并将其引导至位于目标mRNA 3'-非翻译区(3'-UTR)的特定目标位点,从而导致翻译抑制和去甲腺苷酸化诱导的mRNA降解。大多数miRNA是通过RNase III酶Drosha和Dicer的连续作用从发夹结构的前体加工而成的。但是,miR-451的加工不依赖切丁酶,并且切割是由核酸内切酶Ago2介导的。在这里,我们已经表征了miR-451的序列和结构要求,以便处理以及将miRNA分为不同的Ago蛋白。 PremiR-451似乎已针对Ago2裂解进行了优化,并且变化导致处理减少。此外,我们显示,成熟的miR-451仅与Ago2缔合,这表明成熟的miRNA在Ago蛋白家族的不同成员之间不交换。基于与Ago1–3相关的内源性miRNA的克隆和深度测序,我们没有找到在人类细胞中进行miRNA分选的证据。但是,Ago身份似乎会影响某些miRNA的长度,而另一些则不受影响。

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