4.7 Article

A novel motif in the proximal C-terminus of Pannexin 1 regulates cell surface localization

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SCIENTIFIC REPORTS
卷 9, 期 -, 页码 -

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NATURE PORTFOLIO
DOI: 10.1038/s41598-019-46144-5

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资金

  1. Natural Sciences and Engineering Research Council (NSERC) [RGPIN-2017-03889]
  2. Canada Foundation for Innovation (CFI) [29462]
  3. BC Knowledge Development Fund (BCKDF) [804754]
  4. University of Victoria
  5. Michael Smith Foundation for Health Research (MSFHR)
  6. British Columbia Schizophrenia Society Foundation [5900]
  7. UVic Graduate Awards
  8. NSERC [PGSD 459931-2014]
  9. Vanier Canada Graduate Scholarships (NSERC)

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The Pannexin 1 (Panx1) ion and metabolite channel is expressed in a wide variety of cells where it regulates a number of cell behaviours including proliferation and differentiation. Panx1 is expressed on the cell surface as well as intracellular membranes. Previous work suggests that a region within the proximal Panx1 C-terminus (Panx1CT) regulates cell surface localization. Here we report the discovery of a putative leucine-rich repeat (LRR) motif in the proximal Panx1CT necessary for Panx1 cell surface expression in HEK293T cells. Deletion of the putative LRR motif results in significant loss of Panx1 cell surface distribution. Outcomes of complementary cell surface oligomerization and glycosylation state analyses were consistent with reduced cell surface expression of Panx1 LRR deletion mutants. Of note, the oligomerization analysis revealed the presence of putative dimers and trimers of Panx1 at the cell surface. Expression of Panx1 increased HEK293T cell growth and reduced doubling time, while expression of a Panx1 LRR deletion mutant (highly conserved segment) did not reproduce this effect. In summary, here we discovered the presence of a putative LRR motif in the Panx1CT that impacts on Panx1 cell surface localization. Overall these findings provide new insights into the molecular mechanisms underlying C-terminal regulation of Panx1 trafficking and raise potential new lines of investigation with respect to Panx1 oligomerization and glycosylation.

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