4.7 Article

Vps39 Interacts with Tom40 to Establish One of Two Functionally Distinct Vacuole-Mitochondria Contact Sites

期刊

DEVELOPMENTAL CELL
卷 45, 期 5, 页码 621-+

出版社

CELL PRESS
DOI: 10.1016/j.devcel.2018.05.011

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资金

  1. DFG [UN111/10-1, FR 3647/2-1, SFB 894, IRTG 1830]
  2. European Molecular Biology Organization [EMBO ALTF 873-2015]
  3. European Union's Horizon 2020 research and innovation program under the Marie Sklodowska-Curie grant [705853]
  4. Deutsche Forschungsgemeinschaft [BE 4679/2-1, SFB 746]
  5. Deutsche Forschungsgemeinschaft (Research Training Group RTG 2202)
  6. Excellence Initiative of the German Federal Government [EXC 294 BIOSS]
  7. Excellence Initiative of the German State Government [EXC 294 BIOSS]
  8. [Sonderforschungsbereich (SFB) 944]
  9. [SFB 944]
  10. Marie Curie Actions (MSCA) [705853] Funding Source: Marie Curie Actions (MSCA)

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The extensive subcellular network of membrane contact sites plays central roles in organelle biogenesis and communication, yet the precise contributions of the involved machineries remain largely enigmatic. The yeast vacuole forms a membrane contact site with mitochondria, called vacuolar and mitochondrial patch (vCLAMP). Formation of vCLAMPs involves the vacuolar Rab GTPase Ypt7 and the Ypt7-interacting Vps39 subunit of the HOPS tethering complex. Here, we uncover the general preprotein translocase of the outer membrane (TOM) subunit Tom40 as the direct binding partner of Vps39 on mitochondria. We identify Vps39 mutants defective in TOM binding, but functional for HOPS. Cells that cannot form vCLAMPs show reduced growth under stress conditions and impaired survival upon starvation. Unexpectedly, our mutant analysis revealed the existence of two functionally independent vacuole-mitochondria MCSs: one formed by the Ypt7-Vps39-Tom40 tether and a second one by Vps13-Mcp1, which is redundant with ER-mitochondrial contacts formed by ERMES.

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