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Computer simulations of the translocation and unfolding of a protein pulled mechanically through a pore

机译:机械模拟通过孔拉动的蛋白质的移位和展开的计算机模拟

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Protein degradation by ATP-dependent proteases and protein import into the mitochondrial matrix involve the unfolding of proteins upon their passing through narrow constrictions. It has been hypothesized that the cellular machinery accomplishes protein unfolding by pulling mechanically at one end of the polypeptide chain. Here, we use Langevin dynamics simulations of a minimalist off-lattice model to examine this hypothesis and to study the unfolding of a protein domain pulled mechanically through a long narrow pore. We compute the potential of mean force (PMF) experienced by the domain as a function of its displacement along the pore and identify the unfolding intermediates corresponding to the local minima of the PMF. The observed unfolding mechanism is different from that found when the two termini are pulled apart, as in single-molecule mechanical unfolding experiments. It depends on the pore diameter, the magnitude of the pulling force, and on whether the force is applied at the N- or the C-terminus of the chain. Consequently, the translocation time exhibits a pulling force dependence that is more complex than a simple exponential function expected on the basis of simple phenomenological models of translocation. (c) 2005 American Institute of Physics.
机译:由ATP依赖性蛋白酶降解的蛋白质和蛋白质进入线粒体基质的过程包括蛋白质通过狭窄的狭窄区域后的展开。假设细胞机械通过在多肽链的一端机械拉动来完成蛋白质的解折叠。在这里,我们使用极简格子模型的Langevin动力学模拟来检验该假设,并研究通过长而狭窄的孔机械拉伸的蛋白质结构域的展开。我们计算该区域沿孔的位移的函数所对应的平均力(PMF)的潜力,并确定对应于PMF局部最小值的展开中间体。观察到的展开机制与将两个末端拉开时发现的展开机制不同,如在单分子机械展开实验中。它取决于孔径,拉力的大小,以及该力是施加在链的N端还是C端。因此,易位时间表现出的拉力依赖性比根据简单易位现象模型所预期的简单指数函数要复杂得多。 (c)2005年美国物理研究所。

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