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Structure and mechanism of human vesicular polyamine transporter

Nature Communications. 2025-05; 
Yi Guo, Ge Yang, Haijiao Liu, Jin Chai, Jie Chen, John Shanklin, Qun Liu, Bin Liu, Min Lu Center for Proteomics & Molecular Therapeutics, Rosalind Franklin University of Medicine & Science, 3333 Green Bay Road, North Chicago, IL, 60064, USA.
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Gene Synthesis The codon-optimized genes expressing the human VPAT (hVPAT) variants were synthesized by GenScript and sub-cloned into the protein expression vector pFastBac1 at the cloning sites EcoRI and XhoI. Get A Quote

摘要

Polyamines play essential roles in gene expression and modulate neuronal transmission in mammals. Vesicular polyamine transporters (VPAT) from the SLC18 family exploit the transmembrane H+ gradient to translocate polyamines into secretory vesicles, enabling the quantal release of polyamine neuromodulators and underpinning learning and memory formation. Here, we report the cryo-electron microscopy structures of human VPAT in complex with spermine, spermidine, H+, or tetrabenazine, elucidating discrete lumen-facing states of the antiporter and pivotal interactions between VPAT and its substrate or inhibitor. Leveraging structure-inspired mutagenesis studies and protein structure prediction, we deduce an unforesee... More

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