Structural basis of ubiquitin‐independent PP1 complex disassembly by p97

Author:

van den Boom Johannes1,Marini Guendalina2,Meyer Hemmo1ORCID,Saibil Helen R3ORCID

Affiliation:

1. Molecular Biology I, Center of Medical Biotechnology, Faculty of Biology University of Duisburg‐Essen Essen Germany

2. Centre for Structural Systems Biology Leibniz‐Institute of Virology and University Medical Center Hamburg‐Eppendorf (UKE) Hamburg Germany

3. Biological Sciences, Institute of Structural and Molecular Biology Birkbeck University of London London UK

Abstract

AbstractThe AAA+‐ATPase p97 (also called VCP or Cdc48) unfolds proteins and disassembles protein complexes in numerous cellular processes, but how substrate complexes are loaded onto p97 and disassembled is unclear. Here, we present cryo‐EM structures of p97 in the process of disassembling a protein phosphatase‐1 (PP1) complex by extracting an inhibitory subunit from PP1. We show that PP1 and its partners SDS22 and inhibitor‐3 (I3) are loaded tightly onto p97, surprisingly via a direct contact of SDS22 with the p97 N‐domain. Loading is assisted by the p37 adapter that bridges two adjacent p97 N‐domains underneath the substrate complex. A stretch of I3 is threaded into the central channel of the spiral‐shaped p97 hexamer, while other elements of I3 are still attached to PP1. Thus, our data show how p97 arranges a protein complex between the p97 N‐domain and central channel, suggesting a hold‐and‐extract mechanism for p97‐mediated disassembly.

Funder

Wellcome Trust

Publisher

Springer Science and Business Media LLC

Subject

General Immunology and Microbiology,General Biochemistry, Genetics and Molecular Biology,Molecular Biology,General Neuroscience

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