Thioglycoligase derived from fungal GH3 β-xylosidase is a multi-glycoligase with broad acceptor tolerance

Author:

Nieto-Domínguez ManuelORCID,Fernández de Toro Beatriz,de Eugenio Laura I.,Santana Andrés G.,Bejarano-Muñoz LaraORCID,Armstrong ZachORCID,Méndez-Líter Juan Antonio,Asensio Juan Luis,Prieto Alicia,Withers Stephen G.ORCID,Cañada Francisco JavierORCID,Martínez María JesúsORCID

Abstract

AbstractThe synthesis of customized glycoconjugates constitutes a major goal for biocatalysis. To this end, engineered glycosidases have received great attention and, among them, thioglycoligases have proved useful to connect carbohydrates to non-sugar acceptors. However, hitherto the scope of these biocatalysts was considered limited to strong nucleophilic acceptors. Based on the particularities of the GH3 glycosidase family active site, we hypothesized that converting a suitable member into a thioglycoligase could boost the acceptor range. Herein we show the engineering of an acidophilic fungal β-xylosidase into a thioglycoligase with broad acceptor promiscuity. The mutant enzyme displays the ability to form O-, N-, S- and Se- glycosides together with sugar esters and phosphoesters with conversion yields from moderate to high. Analyses also indicate that the pKa of the target compound was the main factor to determine its suitability as glycosylation acceptor. These results expand on the glycoconjugate portfolio attainable through biocatalysis.

Funder

Ministry of Economy and Competitiveness | Agencia Estatal de Investigación

Comunidad de Madrid

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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