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Modulating D-amino acid oxidase (DAAO) substrate specificity through facilitated solvent access

机译:通过促进溶剂接触来调节D-氨基酸氧化酶(DAAO)底物特异性

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摘要

D-amino acid oxidase (DAAO) degrades D-amino acids to produce α-ketoacids, hydrogen peroxide and ammonia. DAAO has often been investigated and engineered for industrial and clinical applications. We combined information from literature with a detailed analysis of the structure to engineer mammalian DAAOs. The structural analysis was complemented with molecular dynamics simulations to characterize solvent accessibility and product release mechanisms. We identified non-obvious residues located on the loops on the border between the active site and the secondary binding pocket essential for pig and human DAAO substrate specificity and activity. We engineered DAAOs by mutating such critical residues and characterised the biochemical activity of the resulting variants. The results highlight the importance of the selected residues in modulating substrate specificity, product egress and enzyme activity, suggesting further steps of DAAO re-engineering towards desired clinical and industrial applications.
机译:D-氨基酸氧化酶(DAAO)降解D-氨基酸以产生α-酮酸,过氧化氢和氨。 DAAO通常已针对工业和临床应用进行了研究和设计。我们将来自文献的信息与对该结构的详细分析相结合,以工程化哺乳动物DAAO。结构分析辅以分子动力学模拟,以表征溶剂可及性和产物释放机理。我们确定了非明显的残基,位于活性位点和次级结合口袋之间的边界上的环上,对猪和人DAAO底物的特异性和活性至关重要。我们通过突变此类关键残基来设计DAAO,并表征了所得变体的生化活性。结果突出了所选残基在调节底物特异性,产物流出和酶活性中的重要性,表明DAAO进一步工程改造以实现所需的临床和工业应用。

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