gp25L/emp24/p24 Protein Family Members of the cis-Golgi Network Bind Both COP I and II Coatomer

Author:

Dominguez Michel1,Dejgaard Kurt1,Füllekrug Joachim1,Dahan Sophie1,Fazel Ali1,Paccaud Jean-Pierre1,Thomas David Y.1,Bergeron John J. M.1,Nilsson Tommy1

Affiliation:

1. Department of Anatomy and Cell Biology, McGill University, Montreal, PQ, H3A2B2, Canada; Cell Biology Programme, European Molecular Biology Laboratory, 69012 Heidelberg, Germany; Genetics Group, Biotechnology Research Institute, National Research Council of Canada, H4P2R2 Montreal, Canada; and Department of Morphology, University of Geneva School of Medicine, 4CH-1211 Geneva, Switzerland

Abstract

Abstract. Five mammalian members of the gp25L/ emp24/p24 family have been identified as major constituents of the cis-Golgi network of rat liver and HeLa cells. Two of these were also found in membranes of higher density (corresponding to the ER), and this correlated with their ability to bind COP I in vitro. This binding was mediated by a K(X)KXX-like retrieval motif present in the cytoplasmic domain of these two members. A second motif, double phenylalanine (FF), present in the cytoplasmic domain of all five members, was shown to participate in the binding of Sec23 (COP II). This motif is part of a larger one, similar to the F/YXXXXF/Y strong endocytosis and putative AP2 binding motif. In vivo mutational analysis confirmed the roles of both motifs so that when COP I binding was expected to be impaired, cell surface expression was observed, whereas mutation of the Sec23 binding motif resulted in a redistribution to the ER. Surprisingly, upon expression of mutated members, steady-state distribution of unmutated ones shifted as well, presumably as a consequence of their observed oligomeric properties.

Publisher

Rockefeller University Press

Subject

Cell Biology

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