The endosomal sorting complex required for transport (ESCRT)-III mediates budding and abscission of intraluminal vesicles (ILVs) into multivesicular endosomes. To further define the role of the ESCRT-III associated protein Mos10/Vps60 in ILV formation, we screened for new interaction partners by SILAC/MS. Here we focused on the newly identified interaction partner Vps68. Our data suggest that Vps68 cooperates with ESCRT-III in ILV formation. The deletion of VPS68 caused a sorting defect similar to the SNF7 deletion, when the cargo load was high. The composition of ESCRT-III was altered, the level of core components was higher and the level of associated proteins was lower in the deletion strain. Our data further indicate that at some point in the functional cycle of ESCRT-III Snf7 could be replaced by Mos10. Vps68 has an unusual membrane topology. Two of its potential membrane helices are amphipathic helices localized to the luminal side of the endosomal membrane. Based on this membrane topology we propose that Vps68 and ESCRT-III cooperate in the abscission step by weakening the luminal and cytosolic leaflets of the bilayer at the abscission site.
Vps68 cooperates with ESCRT-III in intraluminal vesicle formation
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- Funder(s): Deutsche Forschungsgemeinschaft
- Award Id(s): KO 963/8-1
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Sören Alsleben, Ralf Kölling; Vps68 cooperates with ESCRT-III in intraluminal vesicle formation. J Cell Sci 2022; jcs.259743. doi: https://doi.org/10.1242/jcs.259743
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