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进化分析揭示了谷氨酸转运体中钠偶联的起源。

Evolutionary analysis reveals the origin of sodium coupling in glutamate transporters.

作者信息

Reddy Krishna D, Rasool Burha, Akher Farideh Badichi, Kutlešić Nemanja, Pant Swati, Boudker Olga

机构信息

Department of Physiology and Biophysics, Weill Cornell Medical College, New York, NY, USA.

Department of Molecular Medicine, University of South Florida, Tampa, FL, USA.

出版信息

Nat Struct Mol Biol. 2025 Aug 25. doi: 10.1038/s41594-025-01652-z.

Abstract

Secondary active membrane transporters harness the energy of ion gradients to concentrate their substrates. Homologous transporters evolved to couple transport to different ions in response to changing environments and needs. The bases of such diversification and, thus, principles of ion coupling are unexplored. Here, using phylogenetics and ancestral protein reconstruction, we investigated sodium-coupled transport in prokaryotic glutamate transporters, a mechanism ubiquitous across life domains and critical to neurotransmitter recycling in humans by excitatory amino acid transporters from the solute carrier 1 family. By inferring ancestral prokaryotic transporter sequences during a change in the ion-coupling mechanism, we found an evolutionary transition from sodium-dependent to independent substrate binding and transport. Structural and functional experiments on ancestral transporters suggest that the transition involved allosteric mutations, rendering sodium binding dispensable without affecting the ion-binding sites. Allosteric tuning of transporters' energy landscapes might be a widespread route of their functional diversification.

摘要

次级主动膜转运蛋白利用离子梯度的能量来浓缩其底物。同源转运蛋白不断进化,以根据不断变化的环境和需求将转运与不同的离子偶联。这种多样化的基础以及离子偶联的原理尚未得到探索。在这里,我们利用系统发育学和祖先蛋白重建技术,研究了原核生物谷氨酸转运蛋白中的钠偶联转运机制,该机制在所有生命域中普遍存在,并且对于溶质载体1家族中的兴奋性氨基酸转运蛋白在人类神经递质循环中起着关键作用。通过推断离子偶联机制发生变化期间的原核生物祖先转运蛋白序列,我们发现了从钠依赖性底物结合和转运到独立底物结合和转运的进化转变。对祖先转运蛋白的结构和功能实验表明,这种转变涉及变构突变,使得钠结合变得可有可无,而不影响离子结合位点。转运蛋白能量景观的变构调节可能是其功能多样化的广泛途径。

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