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      The polysome-associated proteins Scp160 and Bfr1 prevent P body formation under normal growth conditions.

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          Abstract

          Numerous mRNAs are degraded in processing bodies (P bodies) in Saccharomyces cerevisiae. In logarithmically growing cells, only 0-1 P bodies per cell are detectable. However, the number and appearance of P bodies change once the cell encounters stress. Here, we show that the polysome-associated mRNA-binding protein Scp160 interacts with P body components, such as the decapping protein Dcp2 and the scaffold protein Pat1, presumably, on polysomes. Loss of either Scp160 or its interaction partner Bfr1 caused the formation of Dcp2-positive structures. These Dcp2-positive foci contained mRNA, because their formation was inhibited by the presence of cycloheximide. In addition, Scp160 was required for proper P body formation because only a subset of bona fide P body components could assemble into the Dcp2-positive foci in Δscp160 cells. In either Δbfr1 or Δscp160 cells, P body formation was uncoupled from translational attenuation as the polysome profile remained unchanged. Collectively, our data suggest that Bfr1 and Scp160 prevent P body formation under normal growth conditions.

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          Author and article information

          Journal
          J. Cell. Sci.
          Journal of cell science
          1477-9137
          0021-9533
          May 1 2014
          : 127
          : Pt 9
          Affiliations
          [1 ] Growth & Development, Biozentrum, University of Basel, Klingelbergstrasse 70, 4056 Basel, Switzerland.
          Article
          jcs.142083
          10.1242/jcs.142083
          24569876
          cd848081-ba26-46c2-bb09-9324ceb2a91a
          History

          Endoplasmic reticulum,Processing bodies,Ribonucleotide particles,Saccharomyces cerevisiae,Stress granules,Stress response,Translation,mRNA,mRNA decay,mRNA metabolism,mRNA-binding proteins

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