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二甲双胍与其铜结合特性相关的生物分子作用模式。

Biomolecular mode of action of metformin in relation to its copper binding properties.

作者信息

Repiščák Peter, Erhardt Stefan, Rena Graham, Paterson Martin J

机构信息

Institute of Chemical Sciences, School of Engineering and Physical Sciences, Heriot-Watt University , Edinburgh, United Kingdom EH14 4AS.

出版信息

Biochemistry. 2014 Feb 4;53(4):787-95. doi: 10.1021/bi401444n. Epub 2014 Jan 24.

DOI:10.1021/bi401444n
PMID:24433134
Abstract

Metformin (Metf), the most commonly used type 2 diabetes drug, is known to affect the cellular housekeeping of copper. Recently, we discovered that the structurally closely related propanediimidamide (PDI) shows a cellular behavior different from that of Metf. Here we investigate the binding of these compounds to copper, to compare their binding strength. Furthermore, we take a closer look at the electronic properties of these compounds and their copper complexes such as molecular orbital interactions and electrostatic potential surfaces. Our results clearly show that the copper binding energies cannot alone be the cause of the biochemical differentiation between Metf and PDI. We conclude that other factors such as pKa values and hydrophilicity of the compounds play a crucial role in their cellular activity. Metf in contrast to PDI can occur as an anion in aqueous medium at moderate pH, forming much stronger complexes particularly with Cu(II) ions, suggesting that biguanides but not PDI may induce easy oxidation of Cu(I) ions extracted from proteins. The higher hydrophobicity and the lack of planarity of PDI may further differentiate it from biguanides in terms of their molecular recognition characteristics. These different properties could hold the key to metformin's mitochondrial activity because they suggest that the drug could act at least in part as a pro-oxidant of accessible protein-bound Cu(I) ions.

摘要

二甲双胍(Metf)是最常用的2型糖尿病药物,已知会影响细胞对铜的管理。最近,我们发现结构密切相关的丙二亚胺酰胺(PDI)表现出与Metf不同的细胞行为。在此,我们研究这些化合物与铜的结合情况,以比较它们的结合强度。此外,我们更深入地研究这些化合物及其铜配合物的电子性质,如分子轨道相互作用和静电势表面。我们的结果清楚地表明,铜结合能并非Metf和PDI生化差异的唯一原因。我们得出结论,其他因素,如化合物的pKa值和亲水性,在它们的细胞活性中起着关键作用。与PDI不同,Metf在中等pH值的水性介质中可以以阴离子形式存在,形成更强的配合物,特别是与Cu(II)离子,这表明双胍类药物而非PDI可能会诱导从蛋白质中提取的Cu(I)离子容易氧化。PDI较高的疏水性和缺乏平面性可能在分子识别特征方面进一步使其与双胍类药物区分开来。这些不同的性质可能是二甲双胍线粒体活性的关键,因为它们表明该药物至少部分可以作为可及的蛋白质结合Cu(I)离子的促氧化剂。

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