| Literature DB >> 36113465 |
Xue Guo1, Philip Schmiege2, Tufa E Assafa3, Rong Wang2, Yan Xu1, Linda Donnelly2, Michael Fine2, Xiaodan Ni4, Jiansen Jiang4, Glenn Millhauser5, Liang Feng6, Xiaochun Li7.
Abstract
Lysosomal amino acid efflux by proton-driven transporters is essential for lysosomal homeostasis, amino acid recycling, mTOR signaling, and maintaining lysosomal pH. To unravel the mechanisms of these transporters, we focus on cystinosin, a prototypical lysosomal amino acid transporter that exports cystine to the cytosol, where its reduction to cysteine supplies this limiting amino acid for diverse fundamental processes and controlling nutrient adaptation. Cystinosin mutations cause cystinosis, a devastating lysosomal storage disease. Here, we present structures of human cystinosin in lumen-open, cytosol-open, and cystine-bound states, which uncover the cystine recognition mechanism and capture the key conformational states of the transport cycle. Our structures, along with functional studies and double electron-electron resonance spectroscopic investigations, reveal the molecular basis for the transporter's conformational transitions and protonation switch, show conformation-dependent Ragulator-Rag complex engagement, and demonstrate an unexpected activation mechanism. These findings provide molecular insights into lysosomal amino acid efflux and a potential therapeutic strategy.Entities:
Keywords: DEER; Keywords; Ragulator-Rag complex; X-ray crystallography; cryo-EM; cystinosin; cystinosis; fast adaptation; lysosomal storage disease; lysosomal transporter; membrane protein dynamics
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Year: 2022 PMID: 36113465 PMCID: PMC9530027 DOI: 10.1016/j.cell.2022.08.020
Source DB: PubMed Journal: Cell ISSN: 0092-8674 Impact factor: 66.850