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Please use this identifier to cite or link to this item: http://cmuir.cmu.ac.th/jspui/handle/6653943832/75518
Title: Catalytic and structural insights into a stereospecific and thermostable class II aldolase HpaI from Acinetobacter baumannii
Authors: Pratchaya Watthaisong
Asweena Binlaeh
Aritsara Jaruwat
Narin Lawan
Jirawat Tantipisit
Juthamas Jaroensuk
Litavadee Chuaboon
Jittima Phonbuppha
Ruchanok Tinikul
Pimchai Chaiyen
Penchit Chitnumsub
Somchart Maenpuen
Authors: Pratchaya Watthaisong
Asweena Binlaeh
Aritsara Jaruwat
Narin Lawan
Jirawat Tantipisit
Juthamas Jaroensuk
Litavadee Chuaboon
Jittima Phonbuppha
Ruchanok Tinikul
Pimchai Chaiyen
Penchit Chitnumsub
Somchart Maenpuen
Keywords: Biochemistry, Genetics and Molecular Biology
Issue Date: 1-Nov-2021
Abstract: Aldolases catalyze the reversible reactions of aldol condensation and cleavage and have strong potential for the synthesis of chiral compounds, widely used in pharmaceuticals. Here, we investigated a new Class II metal aldolase from the p-hydroxyphenylacetate degradation pathway in Acinetobacter baumannii, 4-hydroxy-2-keto-heptane-1,7-dioate aldolase (AbHpaI), which has various properties suitable for biocatalysis, including stereoselectivity/stereospecificity, broad aldehyde utilization, thermostability, and solvent tolerance. Notably, the use of Zn2+ by AbHpaI as a native cofactor is distinct from other enzymes in this class. AbHpaI can also use other metal ion (M2+) cofactors, except Ca2+, for catalysis. We found that Zn2+ yielded the highest enzyme complex thermostability (Tm of 87 °C) and solvent tolerance. All AbHpaI·M2+ complexes demonstrated preferential cleavage of (4R)-2-keto-3-deoxy-D-galactonate ((4R)-KDGal) over (4S)-2-keto-3-deoxy-D-gluconate ((4S)-KDGlu), with AbHpaI·Zn2+ displaying the highest R/S stereoselectivity ratio (sixfold higher than other M2+ cofactors). For the aldol condensation reaction, AbHpaI·M2+ only specifically forms (4R)-KDGal and not (4S)-KDGlu and preferentially catalyzes condensation rather than cleavage by ~40-fold. Based on 11 X-ray structures of AbHpaI complexed with M2+ and ligands at 1.85 to 2.0 Å resolution, the data clearly indicate that the M2+ cofactors form an octahedral geometry with Glu151 and Asp177, pyruvate, and water molecules. Moreover, Arg72 in the Zn2+-bound form governs the stereoselectivity/stereospecificity of AbHpaI. X-ray structures also show that Ca2+ binds at the trimer interface via interaction with Asp51. Hence, we conclude that AbHpaI·Zn2+ is distinctive from its homologues in substrate stereospecificity, preference for aldol formation over cleavage, and protein robustness, and is attractive for biocatalytic applications.
URI: https://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=85118931040&origin=inward
http://cmuir.cmu.ac.th/jspui/handle/6653943832/75518
ISSN: 1083351X
00219258
Appears in Collections:CMUL: Journal Articles

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