Argonaute 2/RISC resides in sites of mammalian mRNA decay known as cytoplasmic bodies

Sen, George L.; Blau, Helen M.

doi:10.1038/ncb1265

Cited by 580 publications

(479 citation statements)

References 18 publications

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“…Human Argonaute proteins and C. elegans ALG-1, a worm Argonaute protein required for let-7-directed gene regulation, colocalize, co-purify and interact with proteins also located in PBs (Ding et al, 2005;Jakymiw et al, 2005;Sen and Blau, 2005;Liu et al, 2005a, b;Meister et al, 2005). The localization of Argonaute proteins to PBs requires that the protein bind small RNAs; the target mRNA is transported to the PB only if it contains miRNA-binding sites, suggesting that miRNAs bound to Argonaute proteins direct the mRNA to the PBs (Agbottah et al, 2005;Pillai et al, 2005;Liu et al, 2005a, b).…”

Section: Mechanism(s) Of Mirna-mediated Gene Regulationmentioning

confidence: 99%

Principles and effects of microRNA-mediated post-transcriptional gene regulation

2006

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MicroRNAs (miRNAs) are abundant regulatory RNAs involved in the regulation of many key biological processes. Recent advances in understanding the mechanism of RNA interference and miRNA-mediated mechanisms shed light on major principals of the formation of the regulatory complex and provide models to explain how these small regulatory RNA species interfere with gene expression and how they influence the translational status of the transcriptome.

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Section: Mechanism(s) Of Mirna-mediated Gene Regulationmentioning

confidence: 99%

Principles and effects of microRNA-mediated post-transcriptional gene regulation

2006

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“…Cytoplasmic processing bodies, termed P bodies, are involved in mRNA degradation, nonsense-mediated RNA decay (NMD), siRNA-and micro-RNA (miRNA)-mediated gene silencing in mammalian cells (Sheth and Parker, 2003;Cougot et al, 2004;Jakymiw et al, 2005;Liu et al, 2005aLiu et al, , 2005bSen and Blau, 2005;Bruno and Wilkinson, 2006;Parker and Sheth, 2007). Consistently, P bodies contain components involved in 5' to 3' mRNA degradation, including the decapping complex DCAP1/ DCAP2, decapping coactivators (e.g.…”

Section: Introductionmentioning

confidence: 99%

A genome-wide RNAi screen identifies genes regulating the formation of P bodies in C. elegans and their functions in NMD and RNAi

et al. 2011

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Cytoplasmic processing bodies, termed P bodies, are involved in diverse post-transcriptional processes including mRNA decay, nonsense-mediated RNA decay (NMD), RNAi, miRNA-mediated translational repression and storage of translationally silenced mRNAs. Regulation of the formation of P bodies in the context of multicellular organisms is poorly understood. Here we describe a systematic RNAi screen in C. elegans that identified 224 genes with diverse cellular functions whose inactivations result in a dramatic increase in the number of P bodies. 83 of these genes form a complex functional interaction network regulating NMD. We demonstrate that NMD interfaces with many cellular processes including translation, ubiquitin-mediated protein degradation, intracellular trafficking and cytoskeleton structure. We also uncover an extensive link between translation and RNAi, with different steps in protein synthesis appearing to have distinct effects on RNAi efficiency. Moreover, the intracellular vesicular trafficking network plays an important role in the regulation of RNAi. A subset of genes enhancing P body formation also regulate the formation of stress granules in C. elegans. Our study offers insights into the cellular mechanisms that regulate the formation of P bodies and also provides a framework for system-level understanding of NMD and RNAi in the context of the development of multicellular organisms.

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“…The role of miRNAs in the regulation of gene expression is primarily thought to be through repression of translation, however, there is conflicting evidence as to whether miRNA activity is mediated through effects on the initiation of translation and/or termination [33][34][35]. In addition, miRNA mediated changes in gene expression may also involve RNA cleavage, RNA sequestration and/ or degradation of the transcript to P-bodies [36][37][38][39][40] (Fig. 1).…”

Section: Microrna Biogenesis and Functionmentioning

confidence: 99%

MicroRNAs and genomic instability

Hüppi

Volfovsky

Mackiewicz

et al. 2007

Seminars in Cancer Biology

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A new species of non-coding RNA, microRNAs (miRNAs) has been identified that may regulate the expression of as many as one third to one half of all protein encoding genes. MicroRNAs are found throughout mammalian genomes, but an association between the location of these miRNAs and regions of genomic instability (or fragile sites) in humans has been suggested [1]. In this review we discuss the possible role of altered miRNA expression on human cancer and conduct an analysis correlating the physical location of murine miRNAs with sites of genetic alteration in mouse models of cancer.

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Argonaute 2/RISC resides in sites of mammalian mRNA decay known as cytoplasmic bodies

Cited by 580 publications

References 18 publications

Principles and effects of microRNA-mediated post-transcriptional gene regulation

Principles and effects of microRNA-mediated post-transcriptional gene regulation

A genome-wide RNAi screen identifies genes regulating the formation of P bodies in C. elegans and their functions in NMD and RNAi

MicroRNAs and genomic instability

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