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Model of protein folding: incorporation of a one-dimensional short-range (Ising) model into a three-dimensional model.

机译:蛋白质折叠模型:将一维短程(Ising)模型合并到三维模型中。

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摘要

In this paper, we have incorporated a one-dimensional short-range model into a three-dimensional model for protein folding. It has been applied, by extending the concept of the three-step mechanism for protein folding proposed in our previous paper, to simulate the folding of bovine pancreatic trypsin inhibitor, using a Monte Carlo procedure in all three steps, A, B, and C. The statistical mechanical ensemble treatment of the short-range model serves as a constraint on the Monte Carlo procedure, in which conformational transitions are introduced. The preliminary results of 10 independent Monte Carlo trials indicate that, while folding is achieved, improvements are required in order to account for the correct three-dimensional structure of a globular protein.
机译:在本文中,我们将一维短程模型合并到了蛋白质折叠的三维模型中。通过扩展我们之前论文中提出的蛋白质折叠的三步机制的概念,它已被应用,在三个步骤(A,B和C)中均使用Monte Carlo程序模拟了牛胰胰蛋白酶抑制剂的折叠。短程模型的统计机械合奏处理是对蒙特卡洛过程的约束,其中引入了构象转变。 10个独立的蒙特卡洛试验的初步结果表明,在实现折叠的同时,还需要进行改进,以说明球蛋白的正确三维结构。

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