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首页> 外文期刊>Journal of Molecular Biology >Consensus protein design without phylogenetic bias.
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Consensus protein design without phylogenetic bias.

机译:共识蛋白设计无系统发育偏见。

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摘要

Consensus design is an appealing strategy for the stabilization of proteins. It exploits amino acid conservation in sets of homologous proteins to identify likely beneficial mutations. Nevertheless, its success depends on the phylogenetic diversity of the sequence set available. Here, we show that randomization of a single protein represents a reliable alternative source of sequence diversity that is essentially free of phylogenetic bias. A small number of functional protein sequences selected from binary-patterned libraries suffice as input for the consensus design of active enzymes that are easier to produce and substantially more stable than individual members of the starting data set. Although catalytic activity correlates less consistently with sequence conservation in these extensively randomized proteins, less extreme mutagenesis strategies might be adopted in practice to augment stability while maintaining function.
机译:共识设计是一种稳定蛋白质的诱人策略。它利用同源蛋白质组中的氨基酸保守性来鉴定可能的有益突变。然而,其成功取决于可用序列集的系统发育多样性。在这里,我们显示单个蛋白质的随机化代表了可靠的序列多样性替代来源,该序列多样性基本上没有系统发生偏差。从二元模式文库中选择的少量功能蛋白序列足以作为活性酶共有设计的输入,这些酶比起始数据集的各个成员更易于生产且实质上更稳定。尽管催化活性与这些广泛随机化的蛋白质中的序列保守性不太一致,但是在实践中可以采用较少极端的诱变策略来增强稳定性,同时保持功能。

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