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首页> 外文期刊>Cellular and Molecular Bioengineering >Simulated Thermal Unfolding of the von Willebrand Factor A Domains
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Simulated Thermal Unfolding of the von Willebrand Factor A Domains

机译:von Willebrand Factor A域的模拟热展开

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摘要

The A1 and A2 domains of von Willebrand factor (VWF) have important functions: A1 contains a binding site for platelet glycoprotein Ib (GPIb) while A2 contains a cryptic proteolytic site for the VWF-cleavage enzyme, A Disintegrin And Metalloprotease with a ThromboSpondin type 1 motifs 13 (ADAMTS-13). Because the proteolytic site is fully buried in the native A2 structure, A2 needs to be unfolded to expose its proteolytic site for ADAMTS-13 cleavage. To study the unfolding mechanism of the VWF A domains, we used molecular dynamics (MD) to simulate in atomic details the thermal unfolding of A1 and A2 at high temperatures. The thermal unfolding of A1 and A2 appears very different from their unfolding by tensile forces. At 500 K, unfolding of the central β sheet of A2 starts from the two edges and propagates into the center. β4 and β5 in the center are structurally the most stable and unfolded the latest. However, A2 could be unfolded along different pathways and the unfolded A2 structure is highly flexible. By comparison, A1 is unfolded slower than A2 at 500 K. In even longer time, the unfolding of A1 is limited to the edges of the central β sheet, suggesting a protective role of the N–C terminal disulfide bond.
机译:血管性血友病因子(VWF)的A1和A2结构域具有重要功能:A1包含血小板糖蛋白Ib(GPIb)的结合位点,而A2包含VWF裂解酶,Disintegrin和金属蛋白酶的凝血酶解蛋白类型的隐性蛋白水解位点1个图案13(ADAMTS-13)。由于蛋白水解位点完全掩盖在天然A2结构中,因此A2需要展开以暴露其蛋白水解位点以进行ADAMTS-13切割。为了研究VWF A域的展开机理,我们使用分子动力学(MD)在原子细节上模拟了高温下A1和A2的热展开。 A1和A2的热展开与拉力的展开非常不同。在500 K时,A2的中心β片的展开从两个边缘开始,并传播到中心。中心处的β4和β5在结构上最稳定,并且最新显示。但是,A2可以沿着不同的路径展开,并且展开的A2结构具有高度的灵活性。相比之下,在500 K时,A1的展开比A2慢。在更长的时间内,A1的展开仅限于中央β片的边缘,表明N–C末端二硫键具有保护作用。

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