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首页> 外文期刊>Journal of Molecular Biology >Minimalist protein model as a diagnostic tool for misfolding and aggregation.
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Minimalist protein model as a diagnostic tool for misfolding and aggregation.

机译:极简主义的蛋白质模型可作为错误折叠和聚集的诊断工具。

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We propose a realistic coarse-grained protein model and a technique to "anchor" the model to available experimental data. We apply this procedure to characterize the effect of multiple mutations on the folding mechanism of protein S6. We show that the mutation of a few "gatekeeper" residues triggers significant changes on the folding landscape of S6. These results suggest that gatekeeper residues control the flexibility of critical regions of S6, that in turn regulates the delicate balance between folding and aggregation. Although obtained with a minimalist protein model, these results are fully consistent with experimental evidence and offer a clue to understand the interplay between folding and aggregation in protein S6.
机译:我们提出了一个现实的粗粒蛋白质模型和一种将模型“锚定”到可用实验数据的技术。我们应用此程序来表征多个突变对蛋白质S6折叠机制的影响。我们表明,一些“关守”残基的突变触发S6折叠景观的重大变化。这些结果表明,网守残基控制着S6关键区域的柔韧性,进而调节了折叠和聚集之间的微妙平衡。尽管获得了极简主义的蛋白质模型,但这些结果与实验证据完全一致,并为了解蛋白质S6中折叠与聚集之间的相互作用提供了线索。

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