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从牦牛瘤胃宏基因组中克隆和表征两种β-葡萄糖苷酶/木糖苷酶酶。

Cloning and characterization of two β-glucosidase/xylosidase enzymes from yak rumen metagenome.

机构信息

State Key Laboratory of Genetic Engineering, School of Life Sciences, Fudan University, No. 220 Handan Road, Shanghai, China.

出版信息

Appl Biochem Biotechnol. 2012 Jan;166(1):72-86. doi: 10.1007/s12010-011-9405-x. Epub 2011 Oct 22.

Abstract

Two β-glucosidase/xylosidase genes, Rubg3A and Rubg3B, were cloned from yak rumen uncultured microorganisms by metagenome method and function-based screening. Recombinant RuBG3A and RuBG3B purified from Escherichia coli were characterized for enzymatic properties, and they exhibited activity against 4-nitrophenyl-β-D: -glucopyranoside and 4-nitrophenyl-β-D: -xylopyranoside, suggesting bifunctional β-glucosidase/xylosidase activity. Chromatography analysis showed that they could effectively hydrolyze cellooligosaccharide substrates, indicating the facilitation in saccharification of cellulose. RuBG3A and RuBG3B can also increase the reducing sugar released in xylan hydrolysis to 218% and 169%, respectively, through synergism with xylanase, suggesting their application in hemicellulose saccharification. Molecular modeling and substrate docking showed that there should be one active center responsible for the bifunctional activity in each enzyme, since the active site pocket is substantially wide to allow the entry of both β-glucosidic or β-xylosidic substrates, which elucidated the structure-function relationship in substrate specificities. Therefore, the enzymatic properties, the participation in hydrolysis of cellooligosaccharides, and the synergism with xylanase make RuBG3A and RuBG3B very interesting candidates for saccharification of both cellulose and hemicellulose.

摘要

两个β-葡萄糖苷酶/木糖苷酶基因 Rubg3A 和 Rubg3B 通过宏基因组方法和基于功能的筛选从牦牛瘤胃未培养微生物中克隆。从大肠杆菌中纯化的重组 RuBG3A 和 RuBG3B 的酶学性质进行了表征,它们对 4-硝基苯基-β-D:-葡萄糖吡喃糖苷和 4-硝基苯基-β-D:-木糖苷具有活性,表明具有双功能β-葡萄糖苷酶/木糖苷酶活性。色谱分析表明,它们可以有效地水解纤维寡糖底物,表明有助于纤维素糖化。RuBG3A 和 RuBG3B 还可以通过与木聚糖酶的协同作用,将木聚糖水解中释放的还原糖分别提高到 218%和 169%,这表明它们在半纤维素糖化中的应用。分子建模和底物对接表明,每个酶中都应该有一个负责双功能活性的活性中心,因为活性位点口袋非常宽,可以允许进入β-葡萄糖苷或β-木糖苷底物,这阐明了底物特异性中的结构-功能关系。因此,酶学性质、参与纤维寡糖水解以及与木聚糖酶的协同作用使 RuBG3A 和 RuBG3B 成为纤维素和半纤维素糖化非常有趣的候选酶。

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