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Protein-protein Interfaces

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Many proteins form complexes to carry out their functions, making protein-protein interactions (PPIs) essential for an organism's survival. Most PPIs are stabilized by numerous weak noncovalent chemical forces. The physical shape of the interfaces determines the way two proteins interact. Many globular proteins have closely-matching shapes on their surfaces, which form a large number of weak bonds. Additionally, many PPIs occur between two helices or between a surface cleft and a...
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Amyloid fibrils are aggregates of misfolded proteins.  Under most circumstances, misfolded proteins are either refolded by chaperone proteins or degraded by the proteasome. However, in the case of a mutation or a disease, these proteins can accumulate to form large clusters and often further assemble to form elongated fibers, called fibrils. 
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Proteins are chains of amino acids linked together by peptide bonds. Upon synthesis, a protein folds into a three-dimensional conformation, critical to its biological function. Interactions between its constituent amino acids guide protein folding, and hence the protein structure is primarily dependent on its amino acid sequence.
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Purification and Aggregation of the Amyloid Precursor Protein Intracellular Domain
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凝结体接口可以加速蛋白质聚合.

Chang-Hyun Choi1, Daniel S W Lee1, David W Sanders1

  • 1Department of Chemical and Biological Engineering, Princeton University, Princeton, New Jersey.

Biophysical journal
|October 14, 2023
PubMed
概括
此摘要是机器生成的。

蛋白质p62/SQSTM1的生物分子凝聚物加速了神经退行性疾病中突变的多Q聚合物的形成. 这一过程消耗了自由p62,最终抑制了进一步的凝结和聚合物生长.

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科学领域:

  • 神经退行性疾病研究
  • 生物分子冷凝物物理 生物分子冷凝物物理
  • 蛋白质聚合机制 蛋白质聚合机制

背景情况:

  • 蛋白质聚合物是神经退行性疾病的标志.
  • p62/SQSTM1蛋白质结合和隔离异常蛋白质,可能是通过生物分子凝聚物.
  • 在调节病理性蛋白质聚合方面,p62凝结物的作用尚未完全被理解.

研究的目的:

  • 研究p62凝结物调节突变多Q聚合的物理机制.
  • 在疾病模型中阐明p62凝结和聚合物形成之间的动态相互作用.

主要方法:

  • 使用了一种可诱导光的仿生凝结系统.
  • 研究了p62凝聚物和突变的多Q聚合物之间的相互作用.
  • 分析了聚合物形成对p62阶段行为和蛋白质无处不在的作用.

主要成果:

  • 通过接口介导的封存,p62凝结物增强了突变的多Q聚合物的粗化.
  • 这一过程加速了聚Q的积累成更大的聚合物.
  • 大型聚合物隔离聚基化蛋白质,耗尽自由的p62并抑制进一步的凝结.

结论:

  • 通过接口介导的粗化,p62凝结物可以加速病态蛋白质聚合.
  • 总体粗化和调节性蛋白质阶段行为之间存在动态相互作用.
  • 这种相互作用可能有助于蛋白质聚合疾病的发病和进展.