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深入研究野生型和突变型锌转运蛋白 ZnT8 在人类中的结构-功能关系:一种计算结构生物学方法。

Insights into the structure-function relationship of both wild and mutant zinc transporter ZnT8 in human: a computational structural biology approach.

机构信息

Department of Biotechnology and Bioinformatics, Yogi Vemana University, Kadapa, India.

出版信息

J Biomol Struct Dyn. 2020 Jan;38(1):137-151. doi: 10.1080/07391102.2019.1567391. Epub 2019 Jan 31.

DOI:10.1080/07391102.2019.1567391
PMID:30633652
Abstract

Polymorphism rs13266634 in causes abnormal synthesis, maturation and secretion of insulin, resulting in decrease in efficiency of glucose metabolism and diabetes. encodes Zinc transporter 8 protein (ZnT8). Due to lack of NMR/crystal structures of complete ZnT8 transporter, insights into the structure, function and its interaction with different drugs is still not known. Therefore, methods were adopted in the present studies for predicting three-dimensional structure of ZnT8 transporter via comparative modelling approach and studying the impact of mutation (p.ARG325TRP) on architecture and function via simulation studies. Wild-type protein comprises 15 α-helix and 3 β-strands, while mutant consists of 12 α-helix and 2 β-strands, respectively. Interaction studies of mutant ZnT8 transporter with phytochemicals/drugs screened the best phytochemicals, which can retain the wild-type property. Molecular docking studies reveal that mutant proteins have better binding energy with ligands of LY-2608204, Roseoside, and Luzonoid B. Further molecular dynamic simulation analysis exhibited a strong binding of these ligands with mutant protein and displaying similar behaviour as that of wild type. ALA79, ILE80, and ARG215 are the common interacting amino acids with ligand in all three complexes. As the ligands passed ADMET tests, these may be utilized as anti-diabetic drugs in near future. Although earlier studies have reported anti-diabetic property of LY-2608204 and Roseoside, for the first time, this study reporting Luzonoid B may have anti-diabetic property besides elucidating the structure and functions of ZnT8 transporter.

摘要

多态性 rs13266634 在 导致胰岛素的异常合成、成熟和分泌,从而导致葡萄糖代谢效率降低和糖尿病。 编码锌转运蛋白 8 蛋白(ZnT8)。由于缺乏完整 ZnT8 转运体的 NMR/晶体结构,因此对其结构、功能及其与不同药物的相互作用仍不清楚。因此,本研究采用 方法通过比较建模方法预测 ZnT8 转运体的三维结构,并通过模拟研究研究突变(p.ARG325TRP)对结构和功能的影响。野生型蛋白由 15 个 α-螺旋和 3 个 β-链组成,而突变体分别由 12 个 α-螺旋和 2 个 β-链组成。与筛选出的植物化学物质/药物的突变 ZnT8 转运体相互作用研究,保留了野生型特性的最佳植物化学物质。分子对接研究表明,突变蛋白与 LY-2608204、玫瑰糖苷和 Luzonoid B 的配体具有更好的结合能。进一步的分子动力学模拟分析表明,这些配体与突变蛋白具有很强的结合能力,并表现出与野生型相似的行为。ALA79、ILE80 和 ARG215 是与所有三个复合物中配体相互作用的常见氨基酸。由于这些配体通过了 ADMET 测试,它们可能在不久的将来被用作抗糖尿病药物。尽管早期的研究报道了 LY-2608204 和玫瑰糖苷的抗糖尿病特性,但本研究首次报道了 Luzonoid B 除了阐明 ZnT8 转运体的结构和功能外,可能还具有抗糖尿病特性。

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