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Geometry of alpha and beta protein structures.

机译:α和β蛋白质结构的几何形状。

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摘要

Proteins have a wide array of essential functions: from serving as enzymatic catalysts to protecting the immune system as antibodies. Proteins spontaneously self-organize into specific, folded structures determined by their amino acid sequences and the interaction between molecular forces. Since the 3-dimensional structure into which they fold often relates to the specific function of the protein, much effort has been directed towards methods to predict the folded structure from a given sequence, with the hope of being able to understand protein functions from sequence information.;The protein folding problem can be summarized as the attempt to understand the relationship between a protein sequence and a protein's geometric shape, or fold. Thus, there are two principal problems: given a sequence, what 3-dimensional form will the protein take (forward problem), and given a particular fold, what sequence or sequences code for that form (the inverse problem).;In this work, models that represent folds as continuous structures are explored. Models of the two prevalent motifs in protein folds, alpha helices and beta barrels, are developed using axially deformed tubes and surfaces of revolution. These models are then analyzed and used to develop coordinate models of known and unknown structures.
机译:蛋白质具有多种基本功能:从充当酶促催化剂到保护免疫系统作为抗体。蛋白质自发地自组织成特定的折叠结构,该结构由其氨基酸序列和分子力之间的相互作用决定。由于它们折叠成的3维结构通常与蛋白质的特定功能有关,因此已经进行了很多努力,以从给定序列预测折叠结构的方法,希望能够从序列信息中了解蛋白质的功能。蛋白质折叠问题可以概括为试图理解蛋白质序列与蛋白质的几何形状或折叠之间的关系的尝试。因此,存在两个主要问题:给定序列,蛋白质将采用哪种3维形式(正向问题),以及给定特定的折叠倍数,该序列将编码哪种序列(逆向问题)。 ,探索了代表连续结构的褶皱的模型。使用轴向变形的管子和旋转表面开发了蛋白质折叠中两个普遍的基序模型(α螺旋和β桶)。然后分析这些模型,并将其用于开发已知和未知结构的坐标模型。

著录项

  • 作者

    Shah, Aalok.;

  • 作者单位

    The University of Arizona.;

  • 授予单位 The University of Arizona.;
  • 学科 Applied mathematics.;Biochemistry.
  • 学位 Ph.D.
  • 年度 2015
  • 页码 227 p.
  • 总页数 227
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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