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首页> 外文期刊>Protein engineering design & selection: PEDS >Analysis of galactosemia-linked mutations of GALT enzyme using a computational biology approach.
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Analysis of galactosemia-linked mutations of GALT enzyme using a computational biology approach.

机译:使用计算生物学方法分析半乳糖血症相关的GALT酶突变。

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We describe the prediction of the structural and functional effects of mutations on the enzyme galactose-1-phosphate uridyltransferase related to the genetic disease galactosemia, using a fully computational approach. One hundred and seven single-point mutants were simulated starting from the structural model of the enzyme obtained by homology modeling methods. Several bioinformatics programs were then applied to each resulting mutant protein to analyze the effect of the mutations. The mutations have a direct effect on the active site, or on the dimer assembly and stability, or on the monomer stability. We describe how mutations may exert their effect at a molecular level by altering H-bonds, salt bridges, secondary structure or surface features. The alteration of protein stability, at level of monomer and/or dimer, is the main effect observed. We found an agreement between our results and the functional experimental data available in literature for some mutants. The data and analyses for all the mutants are fully available in the web-accessible database hosted at http://bioinformatica.isa.cnr.it/GALT.
机译:我们使用完整的计算方法,描述了与遗传性疾病半乳糖血症有关的酶半乳糖-1-磷酸尿嘧啶转移酶上突变的结构和功能效应的预测。从通过同源建模方法获得的酶的结构模型开始,模拟了一百零七个单点突变体。然后,将几种生物信息学程序应用于每种产生的突变蛋白,以分析突变的影响。突变对活性位点或对二聚体组装和稳定性或对单体稳定性具有直接影响。我们描述了突变如何通过改变H键,盐桥,二级结构或表面特征在分子水平上发挥作用。在单体和/或二聚体水平上蛋白质稳定性的改变是观察到的主要作用。我们发现我们的结果与文献中某些突变体的功能性实验数据之间存在一致性。所有突变体的数据和分析都可在http://bioinformatica.isa.cnr.it/GALT托管的可通过网络访问的数据库中找到。

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