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首页> 外文期刊>The FEBS journal >Single active-site mutants are sufficient to enhance serine:pyruvate -transaminase activity in an -transaminase
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Single active-site mutants are sufficient to enhance serine:pyruvate -transaminase activity in an -transaminase

机译:单个活性位点突变体足以增强-转氨酶中的丝氨酸:丙酮酸-转氨酶活性

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摘要

We have analyzed the natural evolution of transaminase structure and sequence between an -transaminase serine-pyruvate aminotransferase and an -transaminase from Chromobacteriumviolaceum with 20% sequence identity, and identified the active-site regions that are least conserved structurally. We also show that these structural changes correlate strongly with transaminase substrate specificity during evolution and therefore might normally be presumed to be essential determinants of substrate specificity. However, key residues are often conserved spatially during evolution and yet originate from within a different region of the sequence viastructural reorganizations. In the present study, we also show that -transaminase-type serine-pyruvate aminotransferase activity can be engineered into the CV2025 -transaminase scaffold with any one of many possible single-point mutations at three key positions, without the requirement for significant backbone remodeling, or repositioning of the residue from a different region of sequence. This finding has significant implications for enzyme redesign in which solutions to substrate specificity changes may be found more efficiently than is achieved by engineering in all sequence and structure determinants identified by correlation to substrate specificity.
机译:我们分析了转氨酶丝氨酸-丙酮酸转氨酶和来自紫色小球藻的-转氨酶之间的转氨酶结构和序列的自然进化,其序列同一性小于20%,并确定了结构上保守性最低的活性位点区域。我们还表明,这些结构变化与转氨酶底物特异性在进化过程中密切相关,因此通常可以推测是底物特异性的重要决定因素。然而,关键残基在进化过程中通常在空间上是保守的,但仍通过结构重组起源于序列的不同区域内。在本研究中,我们还表明-转氨酶型丝氨酸丙酮酸氨基转移酶活性可以被工程改造为CV2025-转氨酶支架,并在三个关键位置具有许多可能的单点突变中的任何一个,而无需对骨架进行重大改造,或从不同序列区域重新定位残基。这一发现对酶的重新设计具有重要意义,在酶的重新设计中,与通过工程设计与底物特异性相关而鉴定的所有序列和结构决定簇相比,可以更有效地找到底物特异性变化的解决方案。

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