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A program for prediction of protein secondary structure from nucleotide sequence data: application to histocompatibility antigens.

机译:一种从核苷酸序列数据预测蛋白质二级结构的程序:应用于组织相容性抗原。

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摘要

A computer program is described which, given a nucleotide or an amino acid sequence, outputs protein secondary structure prediction curves as well as hydrophobicity and charged-residue profiles. The program allows for cumulative averaging of properties (secondary structure propensities, hydrophobicity and charge profiles) from several homologous primary structures, a novel concept shown to improve the predictive accuracy. The use of the program is demonstrated on a set of nucleotide and amino acid sequences from human and murine histocompatibility antigens of class I and II. The last extracellular domains of both class I and II antigens (alpha 3 of class I, alpha 2 and beta 2 of class II) and the beta 2-microglobulin domain are predicted to consist of seven anti-parallel beta-strands, in accord with previous claims of homology between these domains and the constant domains of immunoglobulin chains. The remaining extracellular domains are all proposed to form an anti-parallel, four-stranded beta-sheet with one of its faces being covered by alpha-helices and/or structureless segments ("open face sandwiches").
机译:描述了一种计算机程序,给定核苷酸或氨基酸序列,该计算机程序输出蛋白质二级结构预测曲线以及疏水性和带电残基图。该程序可以对几种同源一级结构的性质(二级结构倾向性,疏水性和电荷分布)进行累积平均,这是一种新颖的概念,可提高预测准确性。该程序的使用在I类和II类人类和鼠类组织相容性抗原的一组核苷酸和氨基酸序列上得到证明。 I类和II类抗原的最后一个胞外域(I类的α3,II类的α2和β2)和β2-微球蛋白域预计由七个反平行的β链组成,与这些结构域与免疫球蛋白链的恒定结构域之间具有同源性的先前要求。其余所有胞外结构域均被提议形成反平行的四链β-折叠,其一个表面被α-螺旋和/或无结构链段覆盖(“开放式三明治”)。

著录项

  • 作者

    Novotný, J; Auffray, C;

  • 作者单位
  • 年度 1984
  • 总页数
  • 原文格式 PDF
  • 正文语种 en
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