P bodies and the control of mRNA translation and d...[Mol Cell. 2007]

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1: Mol Cell. 2007 Mar 9;25(5):635-46. Links

P bodies and the control of mRNA translation and degradation.

Parker R, Sheth U.

Howard Hughes Medical Institute, University of Arizona, Tucson, AZ 85721, USA. rrparker@email.arizona.edu

Recent results indicate that many untranslating mRNAs in somatic eukaryotic cells assemble into related mRNPs that accumulate in specific cytoplasmic foci referred to as P bodies. Transcripts associated with P body components can either be degraded or return to translation. Moreover, P bodies are also biochemically and functionally related to some maternal and neuronal mRNA granules. This suggests an emerging model of cytoplasmic mRNA function in which the rates of translation and degradation of mRNAs are influenced by a dynamic equilibrium between polysomes and the mRNPs seen in P bodies. Moreover, some mRNA-specific regulatory factors, including miRNAs and RISC, appear to repress translation and promote decay by recruiting P body components to individual mRNAs.

PMID: 17349952 [PubMed - indexed for MEDLINE]

Protection of specific maternal messenger RNAs by the P body protein CGH-1 (Dhh1/RCK) during Caenorhabditis elegans oogenesis. [J Cell Biol. 2008]
P bodies, stress granules, and viral life cycles. [Cell Host Microbe. 2008]
Evidence of P-body-like structures in Trypanosoma cruzi. [Biochem Biophys Res Commun. 2007]
P bodies: at the crossroads of post-transcriptional pathways. [Nat Rev Mol Cell Biol. 2007]
Deadenylation is prerequisite for P-body formation and mRNA decay in mammalian cells. [J Cell Biol. 2008]
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P bodies and the control of mRNA translation and degradation.

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