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支链淀粉酶多位点工程突变体对埃洛糖和潘糖的新型产物特异性

Novel product specificity toward erlose and panose exhibited by multisite engineered mutants of amylosucrase.

作者信息

Vergès Alizée, Cambon Emmanuelle, Barbe Sophie, Moulis Claire, Remaud-Siméon Magali, André Isabelle

机构信息

Laboratoire d'Ingénierie des Systèmes Biologiques et des Procédés, Université de Toulouse, CNRS, INRA, INSA, Toulouse, 31400, France.

出版信息

Protein Sci. 2017 Mar;26(3):566-577. doi: 10.1002/pro.3106. Epub 2017 Feb 12.

Abstract

A computer-aided engineering approach recently enabled to deeply reshape the active site of N. polysaccharea amylosucrase for recognition of non-natural acceptor substrates. Libraries of variants were constructed and screened on sucrose allowing the identification of 17 mutants able to synthesize molecules from sole sucrose, which are not synthesized by the parental wild-type enzyme. Three of the isolated mutants as well as the new products synthesized were characterized in details. Mutants contain between 7 and 11 mutations in the active site and the new molecules were identified as being a sucrose derivative, named erlose (α-d-glucopyranosyl-(1→4)-α-d-glucopyranosyl-(1→2)-β-d-Fructose), and a new malto-oligosaccharide named panose (α-d-glucopyranosyl-(1→6)-α-d-glucopyranosyl-(1→4)-α-d-Glucose). These product specificities were never reported for none of the amylosucrases characterized to date, nor their engineered variants. Optimization of the production of these trisaccharides of potential interest as sweeteners or prebiotic molecules was carried out. Molecular modelling studies were also performed to shed some light on the molecular factors involved in the novel product specificities of these amylosucrase variants.

摘要

一种计算机辅助工程方法最近能够深度重塑多聚糖栖热放线菌淀粉蔗糖酶的活性位点,以识别非天然受体底物。构建了变体文库,并在蔗糖上进行筛选,从而鉴定出17个能够仅从蔗糖合成分子的突变体,这些分子是亲本野生型酶无法合成的。对分离出的三个突变体以及合成的新产物进行了详细表征。突变体在活性位点含有7至11个突变,新分子被鉴定为一种蔗糖衍生物,名为松二糖(α - d - 吡喃葡萄糖基 - (1→4) - α - d - 吡喃葡萄糖基 - (1→2) - β - d - 果糖),以及一种新的麦芽寡糖,名为潘糖(α - d - 吡喃葡萄糖基 - (1→6) - α - d - 吡喃葡萄糖基 - (1→4) - α - d - 葡萄糖)。这些产物特异性在迄今为止表征的任何淀粉蔗糖酶及其工程变体中均未被报道过。对这些具有潜在甜味剂或益生元分子用途的三糖的生产进行了优化。还进行了分子建模研究,以阐明这些淀粉蔗糖酶变体新产物特异性所涉及的分子因素。

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