A New Group of Glycoside Hydrolase Family 13 α-amylases with an Aberrant Catalytic Triad

Overview

Journal Sci Rep

Specialty Science

Date 2017 Mar 14

PMID 28287181

Citations 21

Authors

Fean D Sarian

Stefan Janecek

Tjaard Pijning

Ihsanawati

Zeily Nurachman

Ocky K Radjasa

Lubbert Dijkhuizen

Dessy Natalia

Marc J E C van der Maarel

Affiliations

Soon will be listed here.

Abstract

α-Amylases are glycoside hydrolase enzymes that act on the α(1→4) glycosidic linkages in glycogen, starch, and related α-glucans, and are ubiquitously present in Nature. Most α-amylases have been classified in glycoside hydrolase family 13 with a typical (β/α)-barrel containing two aspartic acid and one glutamic acid residue that play an essential role in catalysis. An atypical α-amylase (BmaN1) with only two of the three invariant catalytic residues present was isolated from Bacillus megaterium strain NL3, a bacterial isolate from a sea anemone of Kakaban landlocked marine lake, Derawan Island, Indonesia. In BmaN1 the third residue, the aspartic acid that acts as the transition state stabilizer, was replaced by a histidine. Three-dimensional structure modeling of the BmaN1 amino acid sequence confirmed the aberrant catalytic triad. Glucose and maltose were found as products of the action of the novel α-amylase on soluble starch, demonstrating that it is active in spite of the peculiar catalytic triad. This novel BmaN1 α-amylase is part of a group of α-amylases that all have this atypical catalytic triad, consisting of aspartic acid, glutamic acid and histidine. Phylogenetic analysis showed that this group of α-amylases comprises a new subfamily of the glycoside hydrolase family 13.

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