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血红色素抑制 γD-晶体蛋白模型肽的淀粉样纤维形成。

Inhibition of amyloid fibrillation of γD-crystallin model peptide by the cochineal Carmine.

机构信息

Department of Molecular Microbiology and Biotechnology, The Shmunis School of Biomedicine and Cancer Research, Tel Aviv University, 69978 Tel Aviv, Israel.

Department of Ophthalmology, Rambam Health Care Campus, Haifa, Israel; The Ruth and Bruce Rappaport Faculty of Medicine, Technion Israel Institute of Technology, Haifa, Israel.

出版信息

Int J Biol Macromol. 2021 Feb 1;169:342-351. doi: 10.1016/j.ijbiomac.2020.12.106. Epub 2020 Dec 18.

DOI:10.1016/j.ijbiomac.2020.12.106
PMID:33347930
Abstract

γD-crystallin is among the most abundant γ-crystallins in the human eye lens which are essential for preserving its transparency. Aging, and environmental changes, cause crystallins to lose their native soluble structure and aggregate, resulting in the formation of cataract. Current treatment of cataract is surgical removal which is costly. Pharmaceutical therapeutics of cataract is an unmet need. We report a screen for small molecules capable of inhibiting aggregation of human γD-crystallin. Using a highly amyloidogenic hexapeptide model GCWMLY derived from the full-length protein, we screened a library of 68 anthraquinone molecules using ThT fluorescence assay. A leading hit, the cochineal Carmine, effectively reduced aggregation of the model GDC6 peptide in dose dependent manner. Similar effect was observed toward aggregation of the full-length γD-crystallin. Transmission electron microscopy, intrinsic Tryptophan fluorescence and ANS fluorescence assays corroborated these results. Insights obtained from molecular docking suggested that Carmine interaction with monomeric GDC6 involved hydrogen bonding with Ace group, Cys, Met residues and hydrophobic contact with Trp residue. Carmine was non-toxic toward retinal cells in culture. It also reduced ex vivo the turbidity of human extracted cataract material. Collectively, our results indicate that Carmine could be used for developing new therapeutics to treat cataract.

摘要

γD-晶体蛋白是人类眼睛晶状体中含量最丰富的γ-晶体蛋白之一,对于保持其透明度至关重要。衰老和环境变化会导致晶体蛋白失去其天然可溶性结构并聚集,从而导致白内障的形成。目前白内障的治疗方法是手术切除,费用昂贵。治疗白内障的药物疗法是一个未满足的需求。我们报告了一种筛选能够抑制人 γD-晶体蛋白聚集的小分子的方法。使用源自全长蛋白的高度淀粉样的六肽 GCWMLY 作为模型,我们使用 ThT 荧光测定法筛选了 68 种蒽醌分子文库。一个主要的命中化合物,胭脂红,能够有效地剂量依赖性地抑制模型 GDC6 肽的聚集。对全长 γD-晶体蛋白的聚集也观察到类似的效果。透射电子显微镜、内源性色氨酸荧光和 ANS 荧光测定法证实了这些结果。分子对接获得的见解表明,胭脂红与单体 GDC6 的相互作用涉及与 Ace 基团、Cys、Met 残基的氢键以及与 Trp 残基的疏水接触。胭脂红对培养的视网膜细胞无毒。它还降低了人提取白内障材料的体外浊度。总之,我们的结果表明,胭脂红可用于开发治疗白内障的新疗法。

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