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

机译:BLOC-1和BLOC-3通过不同的管状转运载体调节往返于黑素体的VAMP7循环

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摘要

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.
机译:膜内细胞器的成熟需要通过与膜运输中间体融合并将融合因子再循环到其起源部位来进行货物递送。黑素体和其他与溶酶体有关的细胞器是从早期的内体中获得货物的,但是所涉及的融合机制及其循环途径尚不清楚。在这里,我们显示v-SNARE VAMP7介导黑素体与管状运输载体的融合,管状运输载体也携带货物蛋白TYRP1,并且需要BLOC-1形成。使用活细胞成像,我们确定了采用不同管状载体的黑素体中VAMP7回收的途径。回收载体还带有结合VAMP7的支架蛋白VARP和受组织限制的Rab GTPase RAB38。回收载体的形成取决于RAB38交换因子BLOC-3。我们的数据表明,VAMP7介导了BLOC-1依赖性运输载体与黑素体的融合,阐明了从黑素体中的SNARE循环是关键的BLOC-3依赖性步骤,并可能解释了与BLOC-1和BLOC-3缺乏相关的色素沉着表型在Hermansky-Pudlak综合征变种中。

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