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通过修饰中心附近表面残基调节可变鱼腥藻苯丙氨酸解氨酶的pH活性谱

Modulating the pH Activity Profiles of Phenylalanine Ammonia Lyase from Anabaena variabilis by Modification of Center-Near Surface Residues.

作者信息

Zhang Fan, Huang Nan, Zhou Li, Cui Wenjing, Liu Zhongmei, Zhu Longbao, Liu Yi, Zhou Zhemin

机构信息

Key Laboratory of Industrial Biotechnology, Ministry of Education, Jiangnan University, Wuxi, 214122, China.

School of Biological and Chemical Engineering, Anhui Polytechnic University, Wuhu, 241000, China.

出版信息

Appl Biochem Biotechnol. 2017 Nov;183(3):699-711. doi: 10.1007/s12010-017-2458-8. Epub 2017 Mar 25.

Abstract

Phenylalanine ammonia lyase from Anabaena variabilis (Av-PAL) is a candidate for the treatment of phenylketonuria (PKU). However, Av-PAL shows its optimal pH at 8.5 and maintains only 70% of its highest activity when pH decreases to 7.3-7.4 (the condition of human plasma). The objective of the study was to shift its optimal pH by mutating surface amino acid residues which interact with the general base Tyr78. Based on the crystal structure and the online program GETAREA, we selected five sites: Asn69, Glu72, Glu75, Asn89, and Val90. Removing negative charges or introducing positive charges near the general base Tyr78 by mutation, the pH optima were successfully shifted to more acidic range. Especially, the pH optima of E75A, E75L, and E75Q were shifted to 7.5 with 35, 30, and 24% higher specific activities than that of the wild, respectively. Half-lives of E75L and E75Q at 70 °C prolonged to 190 and 180 min from 130 min of the wild, respectively. In addition, the higher resistance to a low pH of 3.5 and protease made E75L a candidate for oral medicine of PKU. This work would improve the therapeutic prospect of Av-PAL and provide guidance in modulating optimal pH of enzymes.

摘要

可变鱼腥藻的苯丙氨酸解氨酶(Av-PAL)是治疗苯丙酮尿症(PKU)的一个候选药物。然而,Av-PAL的最适pH为8.5,当pH降至7.3 - 7.4(人体血浆的pH条件)时,其活性仅维持最高活性的70%。本研究的目的是通过突变与通用碱基Tyr78相互作用的表面氨基酸残基来改变其最适pH。基于晶体结构和在线程序GETAREA,我们选择了五个位点:Asn69、Glu72、Glu75、Asn89和Val90。通过突变在通用碱基Tyr78附近去除负电荷或引入正电荷,成功地将最适pH转移到了更酸性的范围。特别是,E75A、E75L和E75Q的最适pH转移到了7.5,比野生型的比活性分别高35%、30%和24%。E75L和E75Q在70℃的半衰期从野生型的130分钟分别延长至190分钟和180分钟。此外,E75L对低pH 3.5和蛋白酶具有更高的抗性,使其成为PKU口服药物的一个候选药物。这项工作将改善Av-PAL的治疗前景,并为调节酶的最适pH提供指导。

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