The role of the N terminus of lipidated human Atg8-family proteins in cis-membrane association

A multifunctional role of Atg8-family proteins (Atg8 from yeast and human LC3 and GABARAP subfamilies, all referred to here as ATG8s) in macroautophagy/autophagy is carried out by two protein domains, the N-terminal helical domain (NHD) and ubiquitin-like (UBL) domain. Previous studies showed that the NHD of PE-conjugated ATG8s mediates membrane hemifusion via a direct interaction with lipids in trans-membrane association, which would require the NHD in lipidated ATG8s to adopt a solvent-oriented, open, conformation that unmasks a UBL domain surface needed for membrane tethering. A purpose of the closed conformation of the NHD masking the tethering surface on the UBL domain, a conformation seen in the most structures of non-lipidated ATG8s, remained elusive. A recent study by Zhang et al. discussed in this article, showed that the N terminus of lipidated human ATG8s adopts the closed conformation when it interacts with the membrane in cis-membrane association, i.e. with the same membrane ATG8 is anchored to. This finding suggests functions for two distinct conformations of the NHD in lipidated ATG8s and raises questions about determinants controlling cis- or trans-membrane associations of the NHD in ATG8-PE.

Automated summary

ATG8-family proteins play multifunctional roles in autophagy. Lipidated ATG8 proteins have two distinct conformations, closed when interacting with the same membrane and open when mediating trans-membrane interactions. These findings are significant for understanding the interactions between the NHD and membrane in ATG8-PE.