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小RNA介导的基因沉默与内体运输相关。

Silencing by small RNAs is linked to endosomal trafficking.

作者信息

Lee Young Sik, Pressman Sigal, Andress Arlise P, Kim Kevin, White Jamie L, Cassidy Justin J, Li Xin, Lubell Kim, Lim Do Hwan, Cho Ik Sang, Nakahara Kenji, Preall Jonathan B, Bellare Priya, Sontheimer Erik J, Carthew Richard W

机构信息

Department of Biochemistry, Molecular Biology and Cell Biology, Northwestern University, Evanston, IL 60201, USA.

出版信息

Nat Cell Biol. 2009 Sep;11(9):1150-6. doi: 10.1038/ncb1930. Epub 2009 Aug 16.

Abstract

Small RNAs direct RNA-induced silencing complexes (RISCs) to regulate stability and translation of mRNAs. RISCs associated with target mRNAs often accumulate in discrete cytoplasmic foci known as GW-bodies. However, RISC proteins can associate with membrane compartments such as the Golgi and endoplasmic reticulum. Here, we show that GW-bodies are associated with late endosomes (multivesicular bodies, MVBs). Blocking the maturation of MVBs into lysosomes by loss of the tethering factor HPS4 (ref. 5) enhances short interfering RNA (siRNA)- and micro RNA (miRNA)-mediated silencing in Drosophila melanogaster and humans. It also triggers over-accumulation of GW-bodies. Blocking MVB formation by ESCRT (endosomal sorting complex required for transport) depletion results in impaired miRNA silencing and loss of GW-bodies. These results indicate that active RISCs are physically and functionally coupled to MVBs. We further show that MVBs promote the competence of RISCs in loading small RNAs. We suggest that the recycling of RISCs is promoted by MVBs, resulting in RISCs more effectively engaging with small RNA effectors and possibly target RNAs. It may provide a means to enhance the dynamics of RNA silencing in the cytoplasm.

摘要

小RNA引导RNA诱导沉默复合体(RISC)来调控mRNA的稳定性和翻译。与靶标mRNA相关的RISC通常会在称为GW小体的离散细胞质病灶中积累。然而,RISC蛋白可以与高尔基体和内质网等膜区室相关联。在这里,我们表明GW小体与晚期内体(多囊泡体,MVB)相关。通过缺失拴系因子HPS4(参考文献5)来阻断MVB成熟为溶酶体,可增强果蝇和人类中短干扰RNA(siRNA)和微小RNA(miRNA)介导的沉默。这也会引发GW小体的过度积累。通过耗尽ESCRT(运输所需的内体分选复合体)来阻断MVB形成,会导致miRNA沉默受损和GW小体丢失。这些结果表明,活性RISC在物理和功能上与MVB耦合。我们进一步表明,MVB促进RISC加载小RNA的能力。我们认为,MVB促进了RISC的循环利用,从而使RISC更有效地与小RNA效应物以及可能的靶标RNA结合。这可能提供了一种增强细胞质中RNA沉默动态性的方法。

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