AI Article Synopsis

  • VPS37A is a key component of the ESCRT-I complex, necessary for bringing certain ESCRT proteins to the phagophore, which is crucial for closing autophagosomes.
  • The exact process of how VPS37A reaches the phagophore is unclear, but its N-terminal domain interacts with highly curved membranes due to specific motifs around its UEVL domain.
  • Mutations in these interaction motifs disrupt the localization of ESCRT-I to the phagophore, leading to incomplete phagophore closure and impaired autophagy, suggesting that the phagophore's unique shape is important for the assembly of the necessary machinery for autophagosome formation.

Article Abstract

VPS37A, an ESCRT-I complex component, is required for recruiting a subset of ESCRT proteins to the phagophore for autophagosome closure. However, the mechanism by which VPS37A is targeted to the phagophore remains obscure. Here, we demonstrate that the VPS37A N-terminal domain exhibits selective interactions with highly curved membranes, mediated by two membrane-interacting motifs within the disordered regions surrounding its Ubiquitin E2 variant-like (UEVL) domain. Site-directed mutations of residues in these motifs disrupt ESCRT-I localization to the phagophore and result in defective phagophore closure and compromised autophagic flux in vivo, highlighting their essential role during autophagy. In conjunction with the UEVL domain, we postulate that these motifs guide a functional assembly of the ESCRT machinery at the highly curved tip of the phagophore for autophagosome closure. These results advance the notion that the distinctive membrane architecture of the cup-shaped phagophore spatially regulates autophagosome biogenesis.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10942982PMC
http://dx.doi.org/10.1038/s42003-024-06026-7DOI Listing

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