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甲硫氨酸-钌配合物对人胰岛淀粉样多肽纤维形成的影响。

Influence of methionine-ruthenium complex on the fibril formation of human islet amyloid polypeptide.

机构信息

Department of Chemistry, Renmin University of China, Beijing, 100872, China.

出版信息

J Biol Inorg Chem. 2019 Mar;24(2):179-189. doi: 10.1007/s00775-019-01637-6. Epub 2019 Jan 30.

DOI:10.1007/s00775-019-01637-6
PMID:30701360
Abstract

The abnormal aggregation and deposition of human islet amyloid polypeptide (hIAPP) are implicated in the pathogeny of type 2 diabetes mellitus (T2DM). Many aromatic ring-containing Ru complexes inhibit the aggregation of hIAPP. A new Ru complex Ru(bipy)(met)·3HO (1), where bipy is 2,2'-bipyridine and met is methionine, was synthesized and employed to resist the fibril formation of hIAPP and to promote the biocompatibility of metal complexes. Two polypyridyl Ru complexes, namely [Ru(bipy)]Cl(2) and Ru(bipy)Cl(3), were used for comparison. Results reveal that the three Ru complexes can inhibit hIAPP aggregation and depolymerize mature hIAPP fibrils. Interaction studies show that Ru complexes bind to hIAPP through metal coordination, hydrophobic interaction, and other intermolecular forces. The binding of the three compounds is spontaneous and exothermic. The compounds also rescue peptide-induced cytotoxicity to some extent. Similar to 3, the novel methionine-Ru complex 1 exhibits an enhanced inhibitory effect and binding affinity to hIAPP possibly because of the smaller steric hindrance and more profitable molecular configuration of 1 than those of 2. The newly designed amino acid-Ru complex may provide new insights into the treatment of T2DM and related amyloidosis diseases. Methionine-Ru complex effectively impedes the fibril formation of human islet amyloid polypeptide.

摘要

人胰岛淀粉样多肽(hIAPP)的异常聚集和沉积与 2 型糖尿病(T2DM)的发病机制有关。许多含芳香环的 Ru 配合物能抑制 hIAPP 的聚集。我们合成了一种新的 Ru 配合物 Ru(bipy)(met)·3HO(1),其中 bipy 是 2,2'-联吡啶,met 是蛋氨酸,用于抵抗 hIAPP 的纤维形成并提高金属配合物的生物相容性。我们还使用了两种多吡啶 Ru 配合物,即[Ru(bipy)]Cl(2)和 Ru(bipy)Cl(3)进行比较。结果表明,这三种 Ru 配合物都能抑制 hIAPP 聚集并解聚成熟的 hIAPP 纤维。相互作用研究表明,Ru 配合物通过金属配位、疏水性相互作用和其他分子间力与 hIAPP 结合。三种化合物的结合是自发的和放热的。这些化合物还在一定程度上挽救了肽诱导的细胞毒性。与 3 类似,新型蛋氨酸-Ru 配合物 1 对 hIAPP 表现出增强的抑制作用和结合亲和力,这可能是由于 1 的空间位阻较小,分子构象更有利。新设计的氨基酸-Ru 配合物可能为治疗 T2DM 和相关淀粉样变性疾病提供新的思路。蛋氨酸-Ru 配合物能有效阻止人胰岛淀粉样多肽的纤维形成。

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Active-Site Environment of Copper-Bound Human Amylin Relevant to Type 2 Diabetes.
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