An interaction between β′-COP and the ArfGAP, Glo3, maintains post-Golgi cargo recycling

Author:

Xie Boyang12ORCID,Guillem Clara1ORCID,Date Swapneeta S.1ORCID,Cohen Cameron I.1ORCID,Jung Christian1ORCID,Kendall Amy K.12ORCID,Best Jordan T.1ORCID,Graham Todd R.1ORCID,Jackson Lauren P.123ORCID

Affiliation:

1. Department of Biological Sciences, Vanderbilt University 1 , Nashville, TN, USA

2. Center for Structural Biology, Vanderbilt University 2 , Nashville, TN, USA

3. Department of Biochemistry, Vanderbilt University 3 , Nashville, TN, USA

Abstract

The essential COPI coat mediates retrieval of transmembrane proteins at the Golgi and endosomes following recruitment by the small GTPase, Arf1. ArfGAP proteins regulate COPI coats, but molecular details for COPI recognition by ArfGAPs remain elusive. Biochemical and biophysical data reveal how β′-COP propeller domains directly engage the yeast ArfGAP, Glo3, with a low micromolar binding affinity. Calorimetry data demonstrate that both β′-COP propeller domains are required to bind Glo3. An acidic patch on β′-COP (D437/D450) interacts with Glo3 lysine residues located within the BoCCS (binding of coatomer, cargo, and SNAREs) region. Targeted point mutations in either Glo3 BoCCS or β′-COP abrogate the interaction in vitro, and loss of the β′-COP/Glo3 interaction drives Ste2 missorting to the vacuole and aberrant Golgi morphology in budding yeast. These data suggest that cells require the β′-COP/Glo3 interaction for cargo recycling via endosomes and the TGN, where β′-COP serves as a molecular platform to coordinate binding to multiple proteins, including Glo3, Arf1, and the COPI F-subcomplex.

Funder

National Institutes of Health

Pew Charitable Trusts

Publisher

Rockefeller University Press

Subject

Cell Biology

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