Vps60 initiates alternative ESCRT-III filaments

Author:

Pfitzner Anna-Katharina1ORCID,Zivkovic Henry1ORCID,Bernat-Silvestre César1ORCID,West Matt2ORCID,Peltier Tanner2ORCID,Humbert Frédéric1ORCID,Odorizzi Greg2ORCID,Roux Aurélien13ORCID

Affiliation:

1. University of Geneva 1 Department of Biochemistry, , Geneva, Switzerland

2. University of Colorado 2 Department of Molecular Cellular and Developmental Biology, , Boulder, CO, USA

3. National Center of Competence in Research in Chemical Biology, University of Geneva 3 , Geneva, Switzerland

Abstract

Endosomal sorting complex required for transport-III (ESCRT-III) participates in essential cellular functions, from cell division to endosome maturation. The remarkable increase of its subunit diversity through evolution may have enabled the acquisition of novel functions. Here, we characterize a novel ESCRT-III copolymer initiated by Vps60. Membrane-bound Vps60 polymers recruit Vps2, Vps24, Did2, and Ist1, as previously shown for Snf7. Snf7- and Vps60-based filaments can coexist on membranes without interacting as their polymerization and recruitment of downstream subunits remain spatially and biochemically separated. In fibroblasts, Vps60/CHMP5 and Snf7/CHMP4 are both recruited during endosomal functions and cytokinesis, but their localization is segregated and their recruitment dynamics are different. Contrary to Snf7/CHMP4, Vps60/CHMP5 is not recruited during nuclear envelope reformation. Taken together, our results show that Vps60 and Snf7 form functionally distinct ESCRT-III polymers, supporting the notion that diversification of ESCRT-III subunits through evolution is linked to the acquisition of new cellular functions.

Funder

Swiss National Fund

European Research Council

National Institutes of Health

National Institute of General Medical Sciences

Fundación Alfonso Martín Escudero

Publisher

Rockefeller University Press

Subject

Cell Biology

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