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Transient intermediate units in protein folding.

机译:蛋白质折叠中的瞬时中间单元。

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摘要

How a polypeptide chain folds into its final native structure as it comes off the ribosome is the final step in the Central Dogma of biology. A better understanding of this fundamental process may have implications for structure prediction, folding diseases and protein design. Cytochrome c is a well-studied protein folding model. Cytochrome c structure can be broken down into cooperative units of secondary structure, detectable by hydrogen exchange. Cytochrome c folds through the sequential acquisition of these structural units. In two-state folding, these units fail to accumulate and are normally undetectable. This work describes the development of a technique that detects not only the transient population of these units but also the “hidden” kinetic barriers that separate them. The folding pathway of cytochrome c seems to have functional importance. Major conformational changes, such as the alkaline transition, appear to occur through the folding pathway. To facilitate further studies, a recombinant cytochrome c was expressed with high yields in E. coli. Initial hydrogen exchange studies of the modified recombinant protein are described. The last section discusses the generalization of the nucleation-sequential stabilization model.
机译:多肽链从核糖体中脱落时如何折叠成其最终的天然结构是生物学中央教义的最后一步。对这个基本过程的更好理解可能对结构预测,疾病折叠和蛋白质设计有影响。细胞色素c是一个经过充分研究的蛋白质折叠模型。细胞色素c结构可分解为二级结构的协作单元,可通过氢交换来检测。细胞色素c通过顺序获取这些结构单元而折叠。在两个状态的折叠中,这些单元无法累积,通常无法检测到。这项工作描述了一种技术的发展,该技术不仅可以检测这些单元的瞬时填充,而且可以检测到将它们分开的“隐藏”动力学障碍。细胞色素c的折叠途径似乎具有功能重要性。主要的构象变化,例如碱性转变,似乎是通过折叠途径发生的。为便于进一步研究,在大肠杆菌中高表达重组细胞色素c。描述了对修饰的重组蛋白的初步氢交换研究。最后一部分讨论了成核顺序稳定模型的推广。

著录项

  • 作者

    Hoang, Linh Duy.;

  • 作者单位

    University of Pennsylvania.;

  • 授予单位 University of Pennsylvania.;
  • 学科 Biophysics General.
  • 学位 Ph.D.
  • 年度 2003
  • 页码 245 p.
  • 总页数 245
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 生物物理学;
  • 关键词

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