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相关概念视频

Cooperative Allosteric Transitions01:58

Cooperative Allosteric Transitions

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Cooperative allosteric transitions can occur in multimeric proteins, where each subunit of the protein has its own ligand-binding site. When a ligand binds to any of these subunits, it triggers a conformational change that affects the binding sites in the other subunits; this can change the affinity of the other sites for their respective ligands. The ability of the protein to change the shape of its binding site is attributed to the presence of a mix of flexible and stable segments in the...
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Protein Dynamics in Living Cells01:19

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Different fluorescence-based techniques are used to study the protein dynamics in living cells. These techniques include FRAP, FRET, and PET.
Fluorescent recovery after photobleaching (FRAP) is a fluorescent-protein-based detection technique used to quantify protein movement rates within the cell. This method exposes a small portion of the cell to an intense laser beam. The laser beam causes permanent photobleaching of the fluorophore-tagged proteins in the exposed region. As the bleached...
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Binding sites linkages can regulate a protein's function.  For example, enzyme activity is often regulated through a feedback mechanism where the end product of the biochemical process serves as an inhibitor.
Aspartate transcarbamoylase (ATCase) is a cytosolic enzyme that catalyzes the condensation of L-aspartate and carbamoyl phosphate to  N-carbamoyl-L-aspartate. This reaction is the first step in pyrimidine biosynthesis. UTP and CTP, the end products of the pyrimidine synthesis...
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An organism can have thousands of different proteins, and these proteins must cooperate to ensure the health of an organism. Proteins bind to other proteins and form complexes to carry out their functions. Many proteins interact with multiple other proteins creating a complex network of protein interactions.
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相关实验视频

Updated: Mar 23, 2026

Optimization of Synthetic Proteins: Identification of Interpositional Dependencies Indicating Structurally and/or Functionally Linked Residues
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蛋白质的时间相关性预测功能模块和动态

Milo M Lin1,2,3

  • 1Green Center for Molecular, Computational, and Systems Biology, University of Texas Southwestern Medical Center , Dallas, Texas 75390, United States.

Journal of the American Chemical Society
|March 23, 2016
PubMed
概括

蛋白质的功能源于运动的时间, 不仅仅是运动. 一个新的条件活动函数揭示了蛋白质的长距离动态相关性,确定了关键的功能位点.

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科学领域:

  • 生物物理
  • 结构生物学
  • 计算生物学

背景情况:

  • 蛋白质结构和功能之间的关系是复杂的,并没有完全阐明.
  • 现有的方法往往无法捕捉长距离的蛋白内通信,而这种通信不会发生显著的结构变化.

研究的目的:

  • 研究如何在蛋白质动态中编码功能信息.
  • 引入一种新的方法来量化蛋白质运动的时间相关性.

主要方法:

  • 条件活动函数的开发和应用.
  • 对三种蛋白质进行微秒长的原子模拟分析.
  • 在侧链二面角之间计算条件活动.

主要成果:

  • 发现功能信息是编码在蛋白质运动的时间, 而不是运动本身.
  • 使用条件活动函数,在稀疏的侧链对之间证明了长距离动态相关性 (高达7 nm).
  • 观察到短距离 (<1 nm) 的结构相关性,与长距离的动态相关性形成对比.

结论:

  • 条件活动函数有效量化蛋白质动态中的时间相关性.
  • 动态相关性揭示了蛋白质内部的功能模块和异质连接.
  • 这种方法通过关注运动时间,为结构-功能范式提供了新的见解.