通过计算机模拟和体外研究来阐明 Cu2+ 和加兰他敏在淀粉样β(1-42)纤维形成过程中的作用。
In silico and in vitro studies to elucidate the role of Cu2+ and galanthamine as the limiting step in the amyloid beta (1-42) fibrillation process.
机构信息
Laboratorio de Modelado Molecular y Bioinformatica, Escuela Superior de Medicina, Instituto Politécnico Nacional, Plan de San Luis y Díaz Mirón s/n, 11340 México City, D.F., México; Laboratorio de Biofísica y Biocatálisis, Escuela Superior de Medicina, Instituto Politécnico Nacional, Plan de San Luis y Díaz Mirón s/n, 11340 México City, D.F., México.
出版信息
Protein Sci. 2013 Oct;22(10):1320-35. doi: 10.1002/pro.2319. Epub 2013 Aug 19.
The formation of fibrils and oligomers of amyloid beta (Aβ) with 42 amino acid residues (Aβ 1-42 ) is the most important pathophysiological event associated with Alzheimer's disease (AD). The formation of Aβ fibrils and oligomers requires a conformational change from an α-helix to a β-sheet conformation, which is encouraged by the formation of a salt bridge between Asp 23 or Glu 22 and Lys 28. Recently, Cu(2+) and various drugs used for AD treatment, such as galanthamine (Reminyl(®) ), have been reported to inhibit the formation of Aβ fibrils. However, the mechanism of this inhibition remains unclear. Therefore, the aim of this work was to explore how Cu(2+) and galanthamine prevent the formation of Aβ1-42 fibrils using molecular dynamics (MD) simulations (20 ns) and in vitro studies using fluorescence and circular dichroism (CD) spectroscopies. The MD simulations revealed that Aβ1-42 acquires a characteristic U-shape before the α-helix to β-sheet conformational change. The formation of a salt bridge between Asp 23 and Lys 28 was also observed beginning at 5 ns. However, the MD simulations of Aβ 1-42 in the presence of Cu(2+) or galanthamine demonstrated that both ligands prevent the formation of the salt bridge by either binding to Glu 22 and Asp 23 (Cu(2+) ) or to Lys 28 (galanthamine), which prevents Aβ 1-42 from adopting the U-characteristic conformation that allows the amino acids to transition to a β-sheet conformation. The docking results revealed that the conformation obtained by the MD simulation of a monomer from the 1Z0Q structure can form similar interactions to those obtained from the 2BGE structure in the oligomers. The in vitro studies demonstrated that Aβ remains in an unfolded conformation when Cu(2+) and galanthamine are used. Then, ligands that bind Asp 23 or Glu 22 and Lys 28 could therefore be used to prevent β turn formation and, consequently, the formation of Aβ fibrils.
β淀粉样蛋白(Aβ)的 42 个氨基酸残基(Aβ1-42)的纤维和低聚物的形成是与阿尔茨海默病(AD)相关的最重要的病理生理事件。Aβ纤维和低聚物的形成需要从α-螺旋到β-折叠构象的构象变化,这是通过Asp 23 或Glu 22 与Lys 28 之间形成盐桥而得到鼓励的。最近,已经报道了 Cu(2+)和用于 AD 治疗的各种药物(如加兰他敏(Reminyl(®)))抑制 Aβ纤维的形成。然而,这种抑制的机制仍不清楚。因此,本工作的目的是使用分子动力学(MD)模拟(20 ns)和使用荧光和圆二色性(CD)光谱法的体外研究来探索 Cu(2+)和加兰他敏如何防止 Aβ1-42 纤维的形成。MD 模拟表明,Aβ1-42 在α-螺旋到β-折叠构象变化之前先获得特征性的 U 形。还观察到 Asp 23 和 Lys 28 之间盐桥的形成始于 5 ns。然而,在存在 Cu(2+)或加兰他敏的情况下,对 Aβ1-42 的 MD 模拟表明,两种配体都通过与 Glu 22 和 Asp 23(Cu(2+))或与 Lys 28(加兰他敏)结合来防止盐桥的形成,从而防止 Aβ1-42 采用允许氨基酸过渡到β-折叠构象的 U 形特征构象。对接结果表明,从 1Z0Q 结构的单体的 MD 模拟获得的构象可以与在低聚物中从 2BGE 结构获得的构象形成类似的相互作用。体外研究表明,当使用 Cu(2+)和加兰他敏时,Aβ 保持未折叠构象。然后,与 Asp 23 或 Glu 22 和 Lys 28 结合的配体可用于防止β转角的形成,从而防止 Aβ纤维的形成。
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