Molecular dynamics of associative memory hamiltonians for protein tertiary structure recognition

Tetrahedron Computer Methodology Pub Date : 1990-01-01 DOI:10.1016/0898-5529(90)90051-9

Mark S. Friedrichs, Peter G. Wolynes

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引用次数: 18

Abstract

A class of associative memory Hamiltonians for protein tertiary recognition was recently introduced by us. By using a minimization scheme based on molecular dynamics with simulated annealing, we are able to improve and expand upon those initial results. For small proteins lower bound estimates of the Hamiltonians' capacity (the maximum size database for which the Hamiltonian has the ability to reproduce structures) are given; in addition, studies of the dependence of this capacity on various global parameters, such as the choice of sequence encodings, the rate of tolerable mutations in the sequence, and the range of active interactions, are reported. The introduction of the molecular dynamics procedure also permits estimates of the capacity for medium-sized proteins (125–200 residues) to be made. These results demonstrate that the capacity for the simplest realizations of the associative memory Hamiltonians grows as 0.5-0.7N, where N is the number of amino acid residues of the protein to be recalled.

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蛋白质三级结构识别的联想记忆哈密顿子分子动力学

本文介绍了一类用于蛋白质三级识别的联想记忆哈密顿量。通过使用基于分子动力学和模拟退火的最小化方案，我们能够在这些初始结果的基础上改进和扩展。对于小蛋白质，给出了哈密顿量的能力(哈密顿量能够复制结构的最大数据库大小)的下限估计;此外，还研究了这种能力对各种全局参数的依赖性，如序列编码的选择、序列中可容忍的突变率和有效相互作用的范围。分子动力学程序的引入也允许估计中型蛋白质(125-200个残基)的容量。这些结果表明，联想记忆哈密顿量的最简单实现容量在0.5-0.7N时增长，其中N是要回忆的蛋白质的氨基酸残基数。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Tetrahedron Computer Methodology

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