AP-1 and KIF13A coordinate endosomal sorting and positioning during melanosome biogenesis

Author:

Delevoye Cédric11,Hurbain Ilse111,Tenza Danièle111,Sibarita Jean-Baptiste11,Uzan-Gafsou Stéphanie11,Ohno Hiroshi2,Geerts Willie J.C.3,Verkleij Arie J.3,Salamero Jean111,Marks Michael S.4,Raposo Graça111

Affiliation:

1. Structure and Membrane Compartments, Cell and Tissue Imaging Facility (IBiSA), Molecular Mechanisms of Intracellular Transport, and Centre Nationale de la Recherche Scientifique, UMR 144 Institut Curie, Centre de Recherche, Paris F-75248, France

2. Research Center for Allergy and Immunology, RIKEN, Yokohama, Kanagawa 230-0045, Japan

3. Department of Cellular Architecture and Dynamics, Universiteit Utrecht, Utrecht 3584 CH, Netherlands

4. Department of Pathology and Laboratory Medicine, University of Pennsylvania, Philadelphia, PA 19104

Abstract

Specialized cell types exploit endosomal trafficking to deliver protein cargoes to cell type–specific lysosome-related organelles (LROs), but how endosomes are specified for this function is not known. In this study, we show that the clathrin adaptor AP-1 and the kinesin motor KIF13A together create peripheral recycling endosomal subdomains in melanocytes required for cargo delivery to maturing melanosomes. In cells depleted of AP-1 or KIF13A, a subpopulation of recycling endosomes redistributes to pericentriolar clusters, resulting in sequestration of melanosomal enzymes like Tyrp1 in vacuolar endosomes and consequent inhibition of melanin synthesis and melanosome maturation. Immunocytochemistry, live cell imaging, and electron tomography reveal AP-1– and KIF13A-dependent dynamic close appositions and continuities between peripheral endosomal tubules and melanosomes. Our results reveal that LRO protein sorting is coupled to cell type–specific positioning of endosomes that facilitate endosome–LRO contacts and are required for organelle maturation.

Publisher

Rockefeller University Press

Subject

Cell Biology

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