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A study on the flexibility of enzyme active sites

机译:酶活性位点的灵活性研究

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Background: A common assumption about enzyme active sites is that their structures are highly conserved to specifically distinguish between closely similar compounds. However, with the discovery of distinct enzymes with similar reaction chemistries, more and more studies discussing the structural flexibility of the active site have been conducted. Results: Most of the existing works on the flexibility of active sites focuses on a set of pre-selected active sites that were already known to be flexible. This study, on the other hand, proposes an analysis framework composed of a new data collecting strategy, a local structure alignment tool and several physicochemical measures derived from the alignments. The method proposed to identify flexible activesites is highly automated and robust so that more extensive studies will be feasible in the future. The experimental results show the proposed method is (a) consistent with previous works based on manually identified flexible active sites and (b) capable of identifying potentially new flexible active sites. Conclusions: This proposed analysis framework and the former analyses on flexibility have their own advantages and disadvantage, depending on the cause of the flexibility. In this regard, this studyproposes an alternative that complements previous studies and helps to construct a more comprehensive view of the flexibility of enzyme active sites.
机译:背景:关于酶活性部位的常见假设是它们的结构高度保守,以特别区分密切地区的化合物。然而,通过发现具有类似反应化学品的不同酶,已经进行了越来越多的研究,已经进行了讨论活性位点的结构柔韧性。结果:大多数现有的工作方法都对活动站点的灵活性侧重于已知是灵活的一组预选的活动站点。另一方面,本研究提出了由新的数据收集策略,局部结构对准工具和源自对准的几种物理化学测量组成的分析框架。提出识别灵活的活性物质的方法是高度自动化和强大的,因此将来更广泛的研究将是可行的。实验结果表明,所提出的方法是(a)与先前的作品一致,基于手动识别的柔性有源站点和(b)能够识别可能新的灵活活动站点。结论:这一提出的分析框架和前者对灵活性的分析具有自身的优点和劣势,具体取决于灵活性的原因。在这方面,这项研究提供了一种补充以前研究的替代方案,并有助于构建更全面的酶活性位点的灵活性观点。

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