High-throughput screening methods for selecting L-threonine aldolases with improved activity

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More and more, aldolases are being recognized as useful catalysts that carry out the reversible addition of a ketone donor to an aldehyde acceptor in achieving high stereoselectivity. Threonine aldolases catalyze the synthesis of variable P-hydroxy-alpha-amino acids, which are important structural units of various antibiotics and inummosuppressants. However, the enzymatic properties need to be improved to support a broader application to synthetic chemistry. Although directed-evolution is a powerful tool for improving enzymatic properties, the successful outcome depends on the efficiency of screening systems. We designed and proposed two high-throughput screening schemes for selecting L-threonine aldolase mutants with improved properties. These schemes utilized the toxicity of aldehyde, which acts as an acceptor in the aldol condensation. In these schemes, the following occurs: (1) the higher L-threonine aldolase activity reduces the toxic effect of aldehyde, which leads to the survival of the corresponding clone (the positive-selection scheme), and (2) the higher L-threonine aldolase activity produces more toxic aldehyde, which causes the death of the corresponding clone (the negative-selection scheme). According to the positive-selection scheme, we successfully selected L-threonine aldolase mutants with higher activities than the wild-type, from a randomly generated LTA library. (C) 2003 Elsevier B.V. All rights reserved.
Publisher
ELSEVIER SCIENCE BV
Issue Date
2003-12
Language
English
Article Type
Article
Keywords

ALPHA-AMINO ACIDS; DIRECTED EVOLUTION; ORGANIC-SYNTHESIS; CHEMOENZYMATIC SYNTHESIS; CATALYZED REACTION; ESCHERICHIA-COLI; KEY INTERMEDIATE; GENE CLONING; ENZYMES; BIOCATALYSIS

Citation

JOURNAL OF MOLECULAR CATALYSIS B-ENZYMATIC, v.26, no.3-6, pp.265 - 272

ISSN
1381-1177
URI
http://hdl.handle.net/10203/11592
Appears in Collection
CH-Journal Papers(저널논문)
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