Literature DB >> 22095554

Development of thermostable Candida antarctica lipase B through novel in silico design of disulfide bridge.

Quang Anh Tuan Le1, Jeong Chan Joo, Young Je Yoo, Yong Hwan Kim.   

Abstract

Lipase B from Candida antarctica (CalB) is a versatile biocatalyst for various bioconversions. In this study, the thermostability of CalB was improved through the introduction of a new disulfide bridge. Analysis of the B-factors of residue pairs in CalB wild type (CalB-WT) followed by simple flexibility analysis of residues in CalB-WT and its designated mutants using FIRST server were newly proposed to enhance the selective power of two computational tools (MODIP and DbD v1.20) to predict the possible disulfide bonds in proteins for the enhancement of thermostability. Five residue pairs (A162-K308, N169-F304, Q156(-) L163, S50-A273, and S239C-D252C) were chosen and the respective amino acid residues were mutated to cysteine. In the results, CalB A162C-K308C showed greatly improved thermostability while maintaining its catalytic efficiency compared to that of CalB-WT. Remarkably, the temperature at which 50% of its activity remained after 60-min incubation (T⁶⁰₅₀) of CalB A162C_K308C was increased by 8.5°C compared to that of CalB-WT (55 and 46.5°C, respectively). Additionally, the half-life at 50°C of CalB A162C-K308C was 4.5-fold higher than that of CalB-WT (220 and 49 min, respectively). The improvement of thermostability of CalB A162C-K308C was elucidated at the molecular level by molecular dynamics (MD) simulation.
Copyright © 2011 Wiley Periodicals, Inc.

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Year:  2011        PMID: 22095554     DOI: 10.1002/bit.24371

Source DB:  PubMed          Journal:  Biotechnol Bioeng        ISSN: 0006-3592            Impact factor:   4.530


  33 in total

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