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      Time-resolved quantitative proteomics implicates the core snRNP protein SmB together with SMN in neural trafficking.

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          Abstract

          The biogenesis of splicing snRNPs (small nuclear ribonucleoproteins) is a complex process, beginning and ending in the nucleus of the cell but including key stages that take place in the cytoplasm. In particular, the SMN (survival motor neuron) protein complex is required for addition of the core Sm proteins to the snRNP. Insufficiency of SMN results in the inherited neurodegenerative condition, spinal muscular atrophy (SMA). Details of the physical organization of the cytoplasmic stages of snRNP biogenesis are unknown. Here, we use time-resolved quantitative proteomics to identify proteins that associate preferentially with either newly assembled or mature splicing snRNPs. We identified highly mobile SmB protein-trafficking vesicles in neural cells, which are dependent on the cellular levels of SMN and SmB for their morphology and mobility. We propose that these represent a family of related vesicles, some of which play a role in snRNP biogenesis and some that might play more diverse roles in cellular RNA metabolism.

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          Author and article information

          Journal
          J. Cell. Sci.
          Journal of cell science
          1477-9137
          0021-9533
          Feb 15 2014
          : 127
          : Pt 4
          Affiliations
          [1 ] College of Life Sciences, University of Dundee, Dundee DD1 5EH, UK.
          Article
          jcs.137703
          10.1242/jcs.137703
          24357717
          93a7e4a9-41d9-47c5-b361-5bb3dd183653
          History

          SILAC protemics,SMN,Spinal muscular atrophy,Survival of motor neuron protein,Vesicles,snRNPs

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