The role of the AP-1 adaptor complex in outgoing and incoming membrane traffic

Author:

Robinson Margaret S.1ORCID,Antrobus Robin1ORCID,Sanger Anneri1ORCID,Davies Alexandra K.2ORCID,Gershlick David C.1ORCID

Affiliation:

1. University of Cambridge 1 Cambridge Institute for Medical Research, , Cambridge, UK

2. University of Manchester 2 Faculty of Biology, Medicine and Health, School of Biological Sciences, Manchester Academic Health Science Centre, , Manchester, UK

Abstract

The AP-1 adaptor complex is found in all eukaryotes, but it has been implicated in different pathways in different organisms. To look directly at AP-1 function, we generated stably transduced HeLa cells coexpressing tagged AP-1 and various tagged membrane proteins. Live cell imaging showed that AP-1 is recruited onto tubular carriers trafficking from the Golgi apparatus to the plasma membrane, as well as onto transferrin-containing early/recycling endosomes. Analysis of single AP-1 vesicles showed that they are a heterogeneous population, which starts to sequester cargo 30 min after exit from the ER. Vesicle capture showed that AP-1 vesicles contain transmembrane proteins found at the TGN and early/recycling endosomes, as well as lysosomal hydrolases, but very little of the anterograde adaptor GGA2. Together, our results support a model in which AP-1 retrieves proteins from post-Golgi compartments back to the TGN, analogous to COPI’s role in the early secretory pathway. We propose that this is the function of AP-1 in all eukaryotes.

Funder

Wellcome Trust

Cambridge Institute for Medical Research, University of Cambridge

Biotechnology and Biological Sciences Research Council

Royal Society

Publisher

Rockefeller University Press

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