BLOC-1 and BLOC-3 regulate VAMP7 cycling to and from melanosomes via distinct tubular transport carriers.

Amanda Acosta-Ruiz; Anderson; Barlowe; Bennett; Boissy; Bonifacino; Bright; Brooks; Bultema; Bultema; Burgo; Burgo; Cai; Chen; Chiang; Cullinane; Cédric Delevoye; Danglot; Danglot; David J. Owen; Delevoye; Delevoye; Dell’Angelica; Dennis; Di Pietro; Domanska; Dorothy C. Bennett; Elena V. Sviderskaya; Fader; Fader; Gardner; Geoffrey G. Hesketh; Gerondopoulos; Ghiani; Gordon; Graça Raposo; Hesketh; Huang; Huizing; Ilse Hurbain; J. Paul Luzio; Jahn; Jani; Kent; Lane; Loftus; Lopes; Luzio; Marks; Martina; Martinez-Arca; Maryse Romao; McGough; Megan K. Dennis; Meng; Michael S. Marks; Mohrmann; Molino; Morita; Nazarian; Newell-Litwa; Nguyen; Nguyen; Orlow; Osanai; Philip S. Goff; Prekeris; Pryor; Pu; Richmond; Ryder; Salazar; Schäfer; Setty; Setty; Seward; Sitaram; Sitaram; Suzuki; Sviderskaya; Takeuchi; Tamura; Tamura; Theos; Thierry Galli; Vijayasaradhi; Wade; Wang; Wasmeier; Wassmer; Wei; Wei; Yatsu; Zhang

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BLOC-1 and BLOC-3 regulate VAMP7 cycling to and from melanosomes via distinct tubular transport carriers.

Abstract

Endomembrane organelle maturation requires cargo delivery via fusion with membrane transport intermediates and recycling of fusion factors to their sites of origin. Melanosomes and other lysosome-related organelles obtain cargoes from early endosomes, but the fusion machinery involved and its recycling pathway are unknown. Here, we show that the v-SNARE VAMP7 mediates fusion of melanosomes with tubular transport carriers that also carry the cargo protein TYRP1 and that require BLOC-1 for their formation. Using live-cell imaging, we identify a pathway for VAMP7 recycling from melanosomes that employs distinct tubular carriers. The recycling carriers also harbor the VAMP7-binding scaffold protein VARP and the tissue-restricted Rab GTPase RAB38. Recycling carrier formation is dependent on the RAB38 exchange factor BLOC-3. Our data suggest that VAMP7 mediates fusion of BLOC-1-dependent transport carriers with melanosomes, illuminate SNARE recycling from melanosomes as a critical BLOC-3-dependent step, and likely explain the distinct hypopigmentation phenotypes associated with BLOC-1 and BLOC-3 deficiency in Hermansky-Pudlak syndrome variants.This work was supported by grants from the National Institutes of Health, National Eye Institute (R01 EY015625, to M.S. Marks and G. Raposo), National Institute of Arthritis and Musculoskeletal and Skin Diseases (R01 AR048155, to M.S. Marks, and F32 AR062476, to M.K. Dennis), National Institute of General Medical Sciences (R01 GM108807, to M.S. Marks); Fondation pour la Recherche Médicale (to T. Galli); the UK Medical Research Council (G0900113, to J.P. Luzio); and the Wellcome Trust (108429, to E.V. Sviderskaya and D.C. Bennett). This work was also supported by a Canadian Institutes of Health Research Fellowship (to G.G. Hesketh) and a Fondation pour la Recherche Médicale grant from Centre National de la Recherche Scientifique, Institut National de la Santé et de la Recherche Médicale, Institut Curie, and Fondation pour la Recherche Médicale (DEQ20140329491 Team label, to G. Raposo).This is the final version of the article. It first appeared from Rockefeller University Press via http://dx.doi.org/10.1083/jcb.20160509

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