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Site-directed mutagenesis to improve the thermostability of tyrosine phenol-lyase

机译:定向诱变,提高酪氨酸苯酚酶的热稳定性

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3,4-Dihydroxyphenyl-L-alanine (L-DOPA) is the most important antiparkinsonian drug, and tyrosine phenollyase (TPL)-based enzyme catalysis process is one of the most adopted methods on industrial scale production. TPL activity and stability represent the rate-limiting step in L-DOPA synthesis. Here, 25 TPL mutants were predicted, and two were confirmed as exhibiting the highest L-DOPA production and named E313W and E313M. The L-DOPA production from E313W and E313M was 47.5 g/L and 62.1 g/L, which was 110.2 % and 174.8 % higher, respectively, than that observed from wild-type (WT) TPL. The K-m of E313W and E313M showed no apparent decrease, whereas the k(cat) of E313W and E313M improved by 45.5 % and 36.4 %, respectively, relative to WT TPL. Additionally, E313W and E313M displayed improved thermostability, a higher melting temperature, and enhanced affinity between for pyridoxal-5'-phosphate. Structural analysis of the mutants suggested increased stability of the N-terminal region via enhanced interactions between the mutated residues and H317. Application of these mutants in a substrate fed-batch strategy as whole-cell biocatalysts allows realization of a cost-efficient short fermentation period resulting in high L-DOPA yield.
机译:3,4-二羟基苯基-L-丙氨酸(L-DOPA)是最重要的抗原蛋白剂药物,而酪氨酸酚醛酶(TPL)基于酶催化过程是工业规模生产最受采用的方法之一。 TPL活性和稳定性代表了L-DOPA合成的速率限制步骤。这里,预测了25个TPL突变体,并确认了两个表现出最高的L-DOPA生产和命名为E313W和E313M。来自E313W和E313M的L-DOPA产生47.5g / L和62.1g / L,分别比从野生型(WT)TPL观察到的110.2%和174.8%。 E313W和E313M的K-M显示出明显的降低,而E313W的K(猫)和E313M相对于WT TPL分别提高45.5%和36.4%。另外,E313W和E313M显示出改善的热稳定性,较高的熔化温度,并且对吡哆醛-5'-磷酸盐之间的增强亲和力。突变体的结构分析表明,通过增强的残基与H317之间的相互作用提高了N-末端区域的稳定性。作为全细胞生物催化剂在基质喂食策略中的应用允许实现成本有效的短发酵时间,导致高L-DOPA产量。

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