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首页> 外文期刊>Journal of Molecular Biology >Evolvability of yeast protein-protein interaction interfaces
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Evolvability of yeast protein-protein interaction interfaces

机译:酵母蛋白质-蛋白质相互作用界面的可进化性

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The functional importance of protein-protein interactions indicates that there should be strong evolutionary constraint on their interaction interfaces. However, binding interfaces are frequently affected by amino acid replacements. Change due to coevolution within interfaces can contribute to variability but is not ubiquitous. An alternative explanation for the ability of surfaces to accept replacements may be that many residues can be changed without affecting the interaction. Candidates for these types of residues are those that make interchain interaction only through the protein main chain, β-carbon, or associated hydrogen atoms. Since almost all residues have these atoms, we hypothesize that this subset of interface residues may be more easily substituted than those that make interactions through other atoms. We term such interactions "residue type independent." Investigating this hypothesis, we find that nearly a quarter of residues in protein interaction interfaces make exclusively interchain residue-type-independent contacts. These residues are less structurally constrained and less conserved than residues making residue-type-specific interactions. We propose that residue-type- independent interactions allow substitutions in binding interfaces while the specificity of binding is maintained.
机译:蛋白质-蛋白质相互作用的功能重要性表明,它们之间的相互作用界面应存在强大的进化约束。但是,结合界面经常受氨基酸置换影响。由于接口内的协同进化而引起的变化可能会导致变化,但并不是普遍存在的。表面接受替代物的能力的另一种解释可能是可以改变许多残基而不影响相互作用。这些类型残基的候选对象是仅通过蛋白质主链,β-碳或相关氢原子进行链间相互作用的那些。由于几乎所有残基都具有这些原子,因此我们假设界面残基的这一子集可能比通过其他原子进行相互作用的残基更容易被取代。我们称这种相互作用为“与残基类型无关”。在研究这个假设时,我们发现蛋白质相互作用界面中将近四分之一的残基仅构成链间不依赖残基类型的接触。这些残基与进行残基类型特异性相互作用的残基相比,在结构上受约束和保守性较低。我们提出,与残基类型无关的相互作用允许在结合界面中进行取代,同时保持结合的特异性。

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