BLOC-1 Brings Together the Actin and Microtubule Cytoskeletons to Generate Recycling Endosomes

Cedric Delevoye, Xavier Heiligenstein, Lea Ripoll, Floriane Gilles-Marsens, Megan K. Dennis, Ricardo Linares Saldana, Laura Derman, Avanti Gokhale, Etienne Morel, Victor Faundez, Michael S. Marks, Graca Raposo
January, 2016
PDF Source Document DOI

Abstract

Summary Recycling endosomes consist of a tubular network that emerges from vacuolar sorting endosomes and diverts cargoes toward the cell surface, the Golgi, or lysosome-related organelles. How recycling tubules are formed remains unknown. We show that recycling endosome biogenesis requires the protein complex BLOC-1. Mutations in BLOC-1 subunits underlie an inherited disorder characterized by albinism, the Hermansky-Pudlak Syndrome, and are associated with schizophrenia risk. We show here that BLOC-1 coordinates the kinesin KIF13A-dependent pulling of endosomal tubules along microtubules to the Annexin A2/actin-dependent stabilization and detachment of recycling tubules. These components cooperate to extend, stabilize and form tubular endosomal carriers that function in cargo recycling and in the biogenesis of pigment granules in melanocytic cells. By shaping recycling endosomal tubules, our data reveal that dysfunction~of the BLOC-1-KIF13A-Annexin A2 molecular network underlies the pathophysiology of neurological and pigmentary disorders.

Type
Journal article
Publication
Current Biology
Ricardo Linares Saldana
Ricardo Linares Saldana
MD PhD

My research interests include distributed robotics, mobile computing and programmable matter.