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首页> 外文期刊>Journal of Biomolecular Structure and Dynamics >Appendant structure plays an important role in amyloidogenic cystatin dimerization prior to domain swapping
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Appendant structure plays an important role in amyloidogenic cystatin dimerization prior to domain swapping

机译:附加结构在结构域交换之前在淀粉样蛋白半胱氨酸蛋白酶抑制剂二聚作用中起重要作用

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摘要

It has been hypothesized that prior to protein domain swapping, unfolding occurs in regions important for the stability of the native monomeric structure, which probably increases the possibility of intermolecular interaction. In order to explore the detailed information of the important unfolding regions in cystatin prior to domain swapping, 20 ns molecular dynamic simulations were performed at atomic level with typical amyloidogenic chicken cystatin (cC) mutant I66Q monomer under conditions that enable forming amyloid fibrils in biological experiments. Our results showed that I66Q mutant exhibited relatively large secondary structure changes and obvious expanding tendency of hydrophobic core compared to wild-type cC. More importantly, the appendant structure (AS) showed a large displacement and distortion towards the hydrophobic core in amyloidogenic cystatin. The structural analysis on cystatin monomer suggested that structural changes of the AS might make the hydrophobic core expand more easily. In addition, analysis on docking dimer has shown that the distorted AS was favor to intermolecular interactions between two cystatin monomers. Data from an independent theoretical derived algorithm as well as biological experiments also support this hypothesis.
机译:已经假设在蛋白质结构域交换之前,在对于天然单体结构的稳定性重要的区域中发生了解折叠,这可能增加了分子间相互作用的可能性。为了探索域交换之前胱抑素中重要的未折叠区域的详细信息,在生物学实验中,在能够形成淀粉样蛋白原纤维的条件下,对典型的淀粉样蛋白鸡胱抑素(cC)突变体I66Q单体进行了原子级的20 ns分子动力学模拟。 。我们的结果表明,与野生型cC相比,I66Q突变体表现出相对较大的二级结构变化和明显的疏水核扩展趋势。更重要的是,附加结构(AS)在淀粉样蛋白形成的半胱氨酸蛋白酶抑制剂中向疏水核表现出较大的位移和变形。对胱抑素单体的结构分析表明,AS的结构变化可能使疏水核更容易扩展。此外,对接二聚体的分析表明,扭曲的AS有利于两个半胱氨酸蛋白酶抑制剂单体之间的分子间相互作用。来自独立理论推导算法和生物学实验的数据也支持该假设。

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