4.7 Article

An ancient Sec10-formin fusion provides insights into actin-mediated regulation of exocytosis

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JOURNAL OF CELL BIOLOGY
卷 217, 期 3, 页码 945-957

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ROCKEFELLER UNIV PRESS
DOI: 10.1083/jcb.201705084

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资金

  1. National Science Foundation [MCB-1330171]
  2. David and Lucille Packard Foundation
  3. Marine Biologicial Laboratory
  4. Laura and Arthur Colwin Endowed Summer Research Fellowship
  5. Burr and Susie Steinbach Fellowship Funds
  6. Nikon Fellowship
  7. Gilgut Fellowship from the Plant Biology Graduate Program at the University of Massachusetts Amherst
  8. Div Of Molecular and Cellular Bioscience
  9. Direct For Biological Sciences [1824636] Funding Source: National Science Foundation

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Exocytosis, facilitated by the exocyst, is fundamentally important for remodeling cell walls and membranes. Here, we analyzed For1F, a novel gene that encodes a fusion of an exocyst subunit (Sec10) and an actin nucleation factor (formin). We showed that the fusion occurred early in moss evolution and has been retained for more than 170 million years. In Physcomitrella patens, For1F is essential, and the expressed protein is a fusion of Sec10 and formin. Reduction of For1F or actin filaments inhibits exocytosis, and For1F dynamically associates with Sec6, another exocyst subunit, in an actin-dependent manner. Complementation experiments demonstrate that constitutive expression of either half of the gene or the paralogous Sec10b rescues loss of For1F, suggesting that fusion of the two domains is not essential, consistent with findings in yeast, where formin and the exocyst are linked noncovalently. Although not essential, the fusion may have had selective advantages and provides a unique opportunity to probe actin regulation of exocytosis.

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