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Human prion protein binds Argonaute and promotes accumulation of microRNA effector complexes

机译:人类病毒蛋白结合Argonaute并促进microRNA效应物复合物的积累

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摘要

Despite intense research in the context of neurodegenerative diseases associated with its misfolding, the endogenous human prion protein PrP ~C (or PRNP) has poorly understood physiological functions. Whereas most PrP ~C is exposed to the extracellular environment, conserved domains result in transmembrane forms of PrP ~C that traffic in the endolysosomal system and are linked to inherited and infectious neuropathologies. One transmembrane PrP ~C variant orients the N-terminal 'octarepeat' domain into the cytoplasm. Here we demonstrate that the octarepeat domain of human PrP ~C contains GW/WG motifs that bind Argonaute (AGO) proteins, the essential components of microRNA (miRNA)-induced silencing complexes (miRISCs). Transmembrane PrP ~C preferentially binds AGO, and PrP ~C promotes formation or stability of miRISC effector complexes containing the trinucleotide repeat-containing gene 6 proteins (TNRC6) and miRNA-repressed mRNA. Accordingly, effective repression of several miRNA targets requires PrP ~C. We propose that dynamic interactions between PrP ~C-enriched endosomes and subcellular foci of AGO underpin these effects.
机译:尽管在神经退行性疾病与其错误折叠相关的背景下进行了深入研究,但是内源性人类病毒蛋白PrP〜C(或PRNP)对生理功能的了解却很少。尽管大多数PrP〜C暴露于细胞外环境,但保守的结构域会导致跨膜形式的PrP〜C进入溶酶体系统,并与遗传性和感染性神经病理学相关。一种跨膜PrP〜C变体将N末端的“八肽”结构域定向到细胞质中。在这里,我们证明了人类PrP〜C的八面体域包含与Argonaute(AGO)蛋白结合的GW / WG基序,Argonaute(AGO)蛋白是microRNA(miRNA)诱导的沉默复合体(miRISCs)的基本组成部分。跨膜PrP〜C优先结合AGO,而PrP〜C促进含有三核苷酸重复序列基因6蛋白(TNRC6)和miRNA抑制的mRNA的miRISC效应子复合物的形成或稳定性。因此,有效抑制几种miRNA靶标需要PrP〜C。我们提出,富含PrP〜C的内体与AGO亚细胞灶之间的动态相互作用是这些作用的基础。

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