Literature DB >> 25817922

A computational strategy for altering an enzyme in its cofactor preference to NAD(H) and/or NADP(H).

Dongbing Cui1, Lujia Zhang1, Shuiqin Jiang1, Zhiqiang Yao1, Bei Gao1, Jinping Lin1, Y Adam Yuan2, Dongzhi Wei1.   

Abstract

Coenzyme engineering, especially for altered coenzyme specificity, has been a research hotspot for more than a decade. In the present study, a novel computational strategy that enhances the hydrogen-bond interaction between an enzyme and a coenzyme was developed and utilized to alter the coenzyme preference. This novel computational strategy only required the structure of the target enzyme. No other homologous enzymes were needed to achieve alteration in the coenzyme preference of a certain enzyme. Using our novel strategy, Gox2181 was reconstructed from exhibiting complete NADPH preference to exhibiting dual cofactor specificity for NADH and NADPH. Structure-guided Gox2181 mutants were designed in silico and molecular dynamics simulations were performed to evaluate the strength of hydrogen-bond interactions between the enzyme and the coenzyme NADPH. Three Gox2181 mutants displaying high structure stability and structural compatibility to NADH/NADPH were chosen for experimental confirmation. Among the three Gox2181 mutants, Gox2181-Q20R&D43S showed the highest enzymatic activity by utilizing NADPH as its coenzyme, which was even better than the wild-type enzyme. In addition, isothermal titration calorimetry analysis further verified that Gox2181-Q20R&D43S was able to interact with NADPH but the wild-type enzyme could not. This novel computational strategy represents an insightful approach for altering the cofactor preference of target enzymes.
© 2015 FEBS.

Entities:  

Keywords:  altered coenzyme specificity; molecular dynamics simulation; rational computational design; site-directed mutagenesis; structure stability prediction

Mesh:

Substances:

Year:  2015        PMID: 25817922     DOI: 10.1111/febs.13282

Source DB:  PubMed          Journal:  FEBS J        ISSN: 1742-464X            Impact factor:   5.542


  9 in total

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4.  The Important Role of Halogen Bond in Substrate Selectivity of Enzymatic Catalysis.

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Review 5.  Protein Engineering for Nicotinamide Coenzyme Specificity in Oxidoreductases: Attempts and Challenges.

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Review 6.  Protein engineering of oxidoreductases utilizing nicotinamide-based coenzymes, with applications in synthetic biology.

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Authors:  Yao Liu; Yalong Cong; Chuanxi Zhang; Bohuan Fang; Yue Pan; Qiangzi Li; Chun You; Bei Gao; John Z H Zhang; Tong Zhu; Lujia Zhang
Journal:  RSC Adv       Date:  2021-03-24       Impact factor: 3.361

9.  In Vivo Selection for Formate Dehydrogenases with High Efficiency and Specificity toward NADP.

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Journal:  ACS Catal       Date:  2020-06-08       Impact factor: 13.084

  9 in total

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