Characterization of the Mammalian CORVET and HOPS Complexes and Their Modular Restructuring for Endosome Specificity

Publication date

2015-12-18

Authors

van der Kant, Rik
Jonker, Caspar T. H.
Wijdeven, Ruud H.
Bakker, Jeroen
Janssen, Lennert
Klumperman, JudithORCID 0000-0003-4835-6228ISNI 0000000396051744
Neefjes, Jacques

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Supervisors

Document Type

Article

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taverne

Abstract

Trafficking of cargo through the endosomal system depends on endosomal fusion events mediated by SNARE proteins, Rab-GTPases, and multisubunit tethering complexes. The CORVET and HOPS tethering complexes, respectively, regulate early and late endosomal tethering and have been characterized in detail in yeast where their sequential membrane targeting and assembly is well understood. Mammalian CORVET and HOPS subunits significantly differ from their yeast homologues, and novel proteins with high homology to CORVET/HOPS subunits have evolved. However, an analysis of the molecular interactions between these subunits in mammals is lacking. Here, we provide a detailed analysis of interactions within the mammalian CORVET and HOPS as well as an additional endosomal-targeting complex (VIPAS39-VPS33B) that does not exist in yeast. We show that core interactions within CORVET and HOPS are largely conserved but that the membrane-targeting module in HOPS has significantly changed to accommodate binding to mammalian-specific RAB7 interacting lysosomal protein (RILP). Arthrogryposis-renal dysfunction-cholestasis (ARC) syndrome-associated mutations in VPS33B selectively disrupt recruitment to late endosomes by RILP or binding to its partner VIPAS39. Within the shared core of CORVET/HOPS, we find that VPS11 acts as a molecular switch that binds either CORVET-specific TGFBRAP1 or HOPS-specific VPS39/RILP thereby allowing selective targeting of these tethering complexes to early or late endosomes to time fusion events in the endo/lysosomal pathway.

Keywords

AUTOPHAGOSOME-LYSOSOME FUSION, C-VPS COMPLEX, TETHERING COMPLEX, ENDOCYTIC TRAFFICKING, RENAL DYSFUNCTION, MEMBRANE-FUSION, PROTEIN COMPLEX, GTPASE ARL8B, ARC SYNDROME, BIOGENESIS, Taverne

Citation

van der Kant, R, Jonker, C T H, Wijdeven, R H, Bakker, J, Janssen, L, Klumperman, J & Neefjes, J 2015, 'Characterization of the Mammalian CORVET and HOPS Complexes and Their Modular Restructuring for Endosome Specificity', Journal of Biological Chemistry, vol. 290, no. 51, pp. 30280-30290. https://doi.org/10.1074/jbc.M115.688440