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

Authors :
Geoffrey G. Hesketh
David J. Owen
Dorothy C. Bennett
J. Paul Luzio
Michael S. Marks
Graça Raposo
Elena V. Sviderskaya
Cédric Delevoye
Megan K. Dennis
Amanda Acosta-Ruiz
Philip S. Goff
Ilse Hurbain
Thierry Galli
Maryse Romao
Dennis, Megan K [0000-0002-8986-5021]
Acosta-Ruiz, Amanda [0000-0002-7591-4128]
Hurbain, Ilse [0000-0002-0097-7773]
Hesketh, Geoffrey G [0000-0002-5570-7615]
Goff, Philip S [0000-0003-4371-5527]
Sviderskaya, Elena V [0000-0002-4177-8236]
Bennett, Dorothy C [0000-0002-3639-7527]
Luzio, J Paul [0000-0003-3912-9760]
Galli, Thierry [0000-0001-8514-7455]
Marks, Michael S [0000-0001-7435-7262]
Apollo - University of Cambridge Repository
Source :
The Journal of Cell Biology
Publication Year :
2016
Publisher :
Rockefeller University Press, 2016.

Abstract

Dennis et al. analyze cycling of the v-SNARE VAMP7 during melanosome biogenesis in melanocytes. VAMP7 is targeted to and retrieved from maturing melanosomes in separate tubular carriers whose formation requires distinct BLOCs, each defective in variants of Hermansky–Pudlak syndrome.<br />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.

Details

ISSN :
15408140 and 00219525
Volume :
214
Database :
OpenAIRE
Journal :
Journal of Cell Biology
Accession number :
edsair.doi.dedup.....1cb08332738c45352df80194d98b5d17