Literature DB >> 19812249

Dcp1-bodies in mouse oocytes.

Adam Swetloff1, Beatrice Conne, Joachim Huarte, Jean-Luc Pitetti, Serge Nef, Jean-Dominique Vassalli.   

Abstract

Processing bodies (P-bodies) are cytoplasmic granules involved in the storage and degradation of mRNAs. In somatic cells, their formation involves miRNA-mediated mRNA silencing. Many P-body protein components are also found in germ cell granules, such as in mammalian spermatocytes. In fully grown mammalian oocytes, where changes in gene expression depend entirely on translational control, RNA granules have not as yet been characterized. Here we show the presence of P-body-like foci in mouse oocytes, as revealed by the presence of Dcp1a and the colocalization of RNA-associated protein 55 (RAP55) and the DEAD box RNA helicase Rck/p54, two proteins associated with P-bodies and translational control. These P-body-like structures have been called Dcp1-bodies and in meiotically arrested primary oocytes, two types can be distinguished based on their size. They also have different protein partners and sensitivities to the depletion of endogenous siRNA/miRNA and translational inhibitors. However, both type progressively disappear during in vitro meiotic maturation and are virtually absent in metaphase II-arrested secondary oocytes. Moreover, this disassembly of hDcp1a-bodies is concomitant with the posttranslational modification of EGFP-hDcp1a.

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Year:  2009        PMID: 19812249      PMCID: PMC2785738          DOI: 10.1091/mbc.e09-02-0123

Source DB:  PubMed          Journal:  Mol Biol Cell        ISSN: 1059-1524            Impact factor:   4.138


  72 in total

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7.  MicroRNA-dependent localization of targeted mRNAs to mammalian P-bodies.

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  26 in total

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Review 4.  mRNA helicases: the tacticians of translational control.

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Review 6.  RNA granules in germ cells.

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7.  Maternally recruited DCP1A and DCP2 contribute to messenger RNA degradation during oocyte maturation and genome activation in mouse.

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Review 8.  Translational Control in the Latency of Apicomplexan Parasites.

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9.  Distinct subcellular localization and potential role of LINE1-ORF1P in meiotic oocytes.

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10.  KHDC1B is a novel CPEB binding partner specifically expressed in mouse oocytes and early embryos.

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