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人类囊泡多胺转运体的结构与机制

Structure and mechanism of human vesicular polyamine transporter.

作者信息

Guo Yi, Yang Ge, Liu Haijiao, Chai Jin, Chen Jie, Shanklin John, Liu Qun, Liu Bin, Lu Min

机构信息

Center for Proteomics & Molecular Therapeutics, Rosalind Franklin University of Medicine & Science, 3333 Green Bay Road, North Chicago, IL, 60064, USA.

The Hormel Institute, University of Minnesota, 801 16th Ave NE, Austin, MN, 55921, USA.

出版信息

Nat Commun. 2025 May 3;16(1):4142. doi: 10.1038/s41467-025-59549-w.

Abstract

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 unforeseen mechanism whereby the polyamine and H compete for multiple acidic protein residues both directly and indirectly, and rationalize how the antidopaminergic therapeutic tetrabenazine impedes vesicular transport of polyamines. This study unravels the mechanism of an H-coupled polyamine antiporter, reveals mechanistic diversity between VPAT and other SLC18 antiporters, and raises new prospects for combating human disorders of polyamine homeostasis.

摘要

多胺在基因表达中发挥着重要作用,并调节哺乳动物的神经传递。来自SLC18家族的囊泡多胺转运体(VPAT)利用跨膜H梯度将多胺转运到分泌囊泡中,从而实现多胺神经调节剂的量子释放,并支持学习和记忆形成。在此,我们报告了与精胺、亚精胺、H或丁苯那嗪复合的人VPAT的冷冻电子显微镜结构,阐明了反向转运体面向内腔的离散状态以及VPAT与其底物或抑制剂之间的关键相互作用。利用受结构启发的诱变研究和蛋白质结构预测,我们推断出一种意想不到的机制,即多胺和H直接或间接地竞争多个酸性蛋白质残基,并解释了抗多巴胺能治疗药物丁苯那嗪如何阻碍多胺的囊泡运输。这项研究揭示了H偶联多胺反向转运体的机制,揭示了VPAT与其他SLC18反向转运体之间的机制多样性,并为对抗多胺稳态的人类疾病带来了新的前景。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e7d9/12049414/619899f72b0c/41467_2025_59549_Fig1_HTML.jpg

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