Shenzhen Key Labortory of Biomolecular Assembling and Regulation, School of Life Sciences, Southern University of Science and Technology, Shenzhen, 518055, Guangdong, China.
Department of Immunology and Microbiology, School of Life Sciences, Southern University of Science and Technology, Shenzhen, 518055, Guangdong, China.
Nat Commun. 2024 Jun 6;15(1):4811. doi: 10.1038/s41467-024-49204-1.
Human multidrug resistance protein 5 (hMRP5) effluxes anticancer and antivirus drugs, driving multidrug resistance. To uncover the mechanism of hMRP5, we determine six distinct cryo-EM structures, revealing an autoinhibitory N-terminal peptide that must dissociate to permit subsequent substrate recruitment. Guided by these molecular insights, we design an inhibitory peptide that could block substrate entry into the transport pathway. We also identify a regulatory motif, comprising a positively charged cluster and hydrophobic patches, within the first nucleotide-binding domain that modulates hMRP5 localization by engaging with membranes. By integrating our structural, biochemical, computational, and cell biological findings, we propose a model for hMRP5 conformational cycling and localization. Overall, this work provides mechanistic understanding of hMRP5 function, while informing future selective hMRP5 inhibitor development. More broadly, this study advances our understanding of the structural dynamics and inhibition of ABC transporters.
人多药耐药蛋白 5(hMRP5)外排抗癌和抗病毒药物,导致多药耐药。为了揭示 hMRP5 的机制,我们确定了六个不同的冷冻电镜结构,揭示了一个自动抑制的 N 端肽,该肽必须解离以允许随后的底物募集。基于这些分子见解,我们设计了一种抑制肽,可以阻止底物进入运输途径。我们还在第一个核苷酸结合域内鉴定出一个调节基序,该基序由带正电荷的簇和疏水区组成,通过与膜结合来调节 hMRP5 的定位。通过整合我们的结构、生化、计算和细胞生物学发现,我们提出了 hMRP5 构象循环和定位的模型。总的来说,这项工作提供了对 hMRP5 功能的机制理解,同时为未来选择性 hMRP5 抑制剂的开发提供了信息。更广泛地说,这项研究推进了我们对 ABC 转运蛋白结构动力学和抑制的理解。
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