Molecular evolution of Fome lignosus laccase by ethyl methane sulfonate-based random mutagenesis in vitro

Mei-Rong Hu , Ya-Peng Chao , Guo-Qing Zhang , Xiu-Qing Yang , Zhi-Quan Xue , Shi-Jun Qian
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引用次数: 33

Abstract

In order to improve the laccase activity, mutant libraries are constructed through ethyl methane sulfonate-based (EMS) random mutagenesis. Mutagenesis improved expression 3.7-fold to 144 mg l−1 laccase in yeast, together with a 1.4-fold increase in Kcat. Thus, the total activity is enhanced 5-fold for 2,2′-azino-bis 3-ethylbenzothiaoline-6-sulfonic acid (ABTS). In the presence of 0.6 mM copper, the highest activity value reached 30 U ml−1 after a 3-day cultivation at a temperature of 30 °C. In comparison with the wild type, the best mutant enzymatic properties (Km for ABTS and guaiacol, thermo- and pH stability, optimal pH) are not changed. Moreover, amino acid sequence analysis indicates that there are four substitutions in the best mutant laccase (Gly160Asp, Ala167Thr, Gly174Asp, and Glu234Gly). The best mutant laccase model showed that the Gly160 and Ala167 are to be found near the water channel; especially the distance of Ala167 to the Cu3a is 14.46 Å. This implies that it is likely involved in the formation of water channel and that it helps facilitate the easy incoming and outgoing of water.

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甲烷磺酸乙酯随机诱变木质素漆酶的分子进化
为了提高漆酶活性,采用基于甲烷磺酸乙酯(EMS)的随机诱变技术构建了突变体文库。诱变使酵母菌漆酶的表达量增加3.7倍至144mg l−1,Kcat的表达量增加1.4倍。因此,2,2 ' -氮基-双3-乙基苯并噻吩啉-6-磺酸(ABTS)的总活性提高了5倍。在0.6 mM铜的存在下,在30°C的温度下培养3天后,活性值最高达到30 U ml−1。与野生型相比,最佳突变体酶学性能(ABTS和愈创木酚的Km,热稳定性和pH稳定性,最佳pH)没有改变。此外,氨基酸序列分析表明,最佳突变体漆酶有4个取代位点(Gly160Asp、Ala167Thr、Gly174Asp和Glu234Gly)。最佳突变型漆酶模型显示Gly160和Ala167出现在水渠附近;特别是Ala167到Cu3a的距离是14.46 Å。这意味着它可能参与了水渠的形成,并有助于水的容易进出。
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Editorial Board Advances in SELEX and application of aptamers in the central nervous system CIDB: Chlamydia Interactive Database for cross-querying genomics, transcriptomics and proteomics data Direct haplotyping of bi-allelic SNPs using ARMS and RFLP analysis techniques Molecular evolution of Fome lignosus laccase by ethyl methane sulfonate-based random mutagenesis in vitro
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