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Stabilization of Bovine carbonic anhydrase II through rational site-specific immobilization

Authors
Lee, Chang HyunJang, Eui KyoungYeon, Young JooPack, Seung Pil
Issue Date
15-10월-2018
Publisher
ELSEVIER SCIENCE BV
Keywords
Carbonic anhydrase; Site-specific immobilization; Enzyme stability; Quasi-rigid domain analysis; Enzyme flexibility
Citation
BIOCHEMICAL ENGINEERING JOURNAL, v.138, pp.29 - 36
Indexed
SCIE
SCOPUS
Journal Title
BIOCHEMICAL ENGINEERING JOURNAL
Volume
138
Start Page
29
End Page
36
URI
https://scholar.korea.ac.kr/handle/2021.sw.korea/72477
DOI
10.1016/j.bej.2018.06.019
ISSN
1369-703X
Abstract
Carbonic anhydrase (CA) is a prominent biocatalyst used for the enzymatic CO2 capture process. For industrial applications, the immobilization of enzyme on a matrix support is a useful technique for stabilizing the enzyme and improving its reusability. Although there have been several trials for immobilization of CA, there is no systematic approach to investigate which site-specific immobilization is more effective for stabilization of CA. In this study, we investigated the effect of the immobilization position on the stability of CA using a-type Bovine CA (bCAII). Six candidate residues (K9, K36, T85, 0151, E233, or N252) were selected and each Cys mutant was site-specifically immobilized on the magnetic beads. The thermal and long-term stabilities were compared. Interestingly, the immobilized K9C and K36C, in which the immobilized sites are located close to the N-terminus of bCAll, showed 4.0- and 9.8-fold enhanced thermostability, respectively, at 58 degrees C. They also maintained 60.6% and 55.5% of activity, respectively, at 45 degrees C after 20 days, when the wild-type bCAII (free and randomly immobilized) completely lost its activity. These results indicated that the site-specific immobilization of the flexible residues on the N-terminal region could be an effective strategy for the stabilization of bCAll, which would be useful guidelines for the immobilization of other CAs in a site-specific manner. (C) 2018 Elsevier B.V. All rights reserved.
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