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引导RNA序列决定了AGO沉默复合体的切割动力学和构象动力学。

The guide RNA sequence dictates the slicing kinetics and conformational dynamics of the Argonaute silencing complex.

作者信息

Wang Peter Y, Bartel David P

机构信息

Whitehead Institute for Biomedical Research, 455 Main Street, Cambridge, MA, 02142, USA.

Howard Hughes Medical Institute, Cambridge, MA, 02142, USA.

出版信息

bioRxiv. 2024 Jun 20:2023.10.15.562437. doi: 10.1101/2023.10.15.562437.

Abstract

The RNA-induced silencing complex (RISC), which powers RNA interference (RNAi), consists of a guide RNA and an Argonaute protein that slices target RNAs complementary to the guide. We find that for different guide-RNA sequences, slicing rates of perfectly complementary, bound targets can be surprisingly different (>250-fold range), and that faster slicing confers better knockdown in cells. Nucleotide sequence identities at guide-RNA positions 7, 10, and 17 underlie much of this variation in slicing rates. Analysis of one of these determinants implicates a structural distortion at guide nucleotides 6-7 in promoting slicing. Moreover, slicing directed by different guide sequences has an unanticipated, 600-fold range in 3'-mismatch tolerance, attributable to guides with weak (AU-rich) central pairing requiring extensive 3' complementarity (pairing beyond position 16) to more fully populate the slicing-competent conformation. Together, our analyses identify sequence determinants of RISC activity and provide biochemical and conformational rationale for their action.

摘要

驱动RNA干扰(RNAi)的RNA诱导沉默复合体(RISC)由一条向导RNA和一个Argonaute蛋白组成,该蛋白可切割与向导互补的靶RNA。我们发现,对于不同的向导RNA序列,完全互补的结合靶标的切割速率可能会有惊人的差异(超过250倍的范围),并且更快的切割在细胞中能实现更好的基因敲低效果。向导RNA第7、10和17位核苷酸序列的一致性是造成切割速率这种变化的主要原因。对其中一个决定因素的分析表明,向导核苷酸6 - 7处的结构扭曲促进了切割。此外,不同向导序列指导的切割在3'端错配耐受性方面有出乎意料的600倍范围差异,这是由于具有弱(富含AU)中心配对的向导需要广泛的3'端互补(超过第16位的配对)才能更充分地形成有切割能力的构象。总之,我们的分析确定了RISC活性的序列决定因素,并为它们的作用提供了生化和构象方面的理论依据。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0aae/11195417/5b9aaa31cd7d/nihpp-2023.10.15.562437v3-f0001.jpg

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