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Generation and statistical modeling of active protein chimeras: A sequence based approach.

机译:活性蛋白嵌合体的产生和统计建模:一种基于序列的方法。

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摘要

Generation of active protein chimeras is a valuable tool to probe the functional space of proteins. Statistical modeling is the next logical step, allowing us to build a model of gene fragment replaceability between species. In this thesis I begin to develop the statistical tools that are needed to systematically describe combinatorial protein libraries. I present three sets of diverse chimeric protein libraries developed using sequence information. The statistical model of the human N-Ras and human K-Ras-4B genes reveal a set previously unidetifed surface residues on the N-Ras G-Domain that may be involved in cellular localization. Statistical modeling of a library of chimeric proteins between A. thaliana cinnamate 4-hydroxylase (AtC4H) and S. moellendorffii cinnamate 4-hydroxylase (SmC4H) reveal a possible stabilizing effect of the N-terminal amino acids from SmC4H and, irreplaceable catalytic domains between AtC4H and SmC4H. I also show gene fragment replaceability on a small scale between functionally divergent AtC4H and A. thaliana ferulate 5-hyrdoxylase proteins. Finally, I show that commonly occurring residue pairs in the sequence record are effective covariates when modeling activity in the AtC4H-SmC4H chimeric library.
机译:活性蛋白质嵌合体的产生是探测蛋白质功能空间的有价值的工具。统计建模是下一步的逻辑步骤,使我们能够建立物种之间基因片段可替换性的模型。在本文中,我开始开发系统地描述组合蛋白文库所需的统计工具。我介绍了使用序列信息开发的三套不同的嵌合蛋白文库。人类N-Ras和人类K-Ras-4B基因的统计模型揭示了N-Ras G域上一组先前未识别的表面残基,可能与细胞定位有关。拟南芥肉桂酸4-羟化酶(AtC4H)和莫氏小孢子肉桂酸4-羟化酶(SmC4H)之间的嵌合蛋白文库的统计模型表明,SmC4H的N末端氨基酸可能具有稳定作用,并且之间存在不可替代的催化结构域AtC4H和SmC4H。我还显示了在功能不同的AtC4H和拟南芥阿魏酸5-羟化酶蛋白之间的小规模基因片段可替换性。最后,我证明了在AtC4H-SmC4H嵌合文库中对活性进行建模时,序列记录中常见的残基对是有效的协变量。

著录项

  • 作者

    Fico, Nicholas Justin.;

  • 作者单位

    Purdue University.;

  • 授予单位 Purdue University.;
  • 学科 Biology Molecular.;Statistics.
  • 学位 Ph.D.
  • 年度 2013
  • 页码 180 p.
  • 总页数 180
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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