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A plasmid borne, functionally novel glycoside hydrolase family 30 subfamily 8 endoxylanase from solventogenic em>Clostridium/em>

机译:一种质粒,功能性新的糖苷水解酶30亚家族8内氧基酶,来自溶剂型& / em>

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摘要

Glycoside hydrolase family 30 subfamily 8 (GH30-8) β-1,4-endoxylanases are known for their appendage-dependent function requiring recognition of an α-1,2-linked glucuronic acid (GlcA) common to glucuronoxylans for hydrolysis. Structural studies have indicated that the GlcA moiety of glucuronoxylans is coordinated through six hydrogen bonds and a salt bridge. These GlcA-dependent endoxylanases do not have significant activity on xylans that do not bear GlcA substitutions such as unsubstituted linear xylooligosaccharides or cereal bran arabinoxylans. In the present study, we present the structural and biochemical characteristics of xylanase 30A from Clostridium acetobutylicum ( Ca Xyn30A) which was originally selected for study due to predicted structural differences within the GlcA coordination loops. Amino acid sequence comparisons indicated that this Gram-positive-derived GH30-8 more closely resembles Gram-negative derived forms of these endoxylanases: a hypothesis borne out in the developed crystallographic structure model of the Ca Xyn30A catalytic domain ( Ca Xyn30A-CD). Ca Xyn30A-CD hydrolyzes xylans to linear and substituted oligoxylosides showing the greatest rate with the highly arabinofuranose (Ara f )-substituted cereal arabinoxylans. Ca Xyn30A-CD hydrolyzes xylooligosaccharides larger than xylotriose and shows an increased relative rate of hydrolysis for xylooligosaccharides containing α-1,2-linked arabinofuranose substitutions. Biochemical analysis confirms that Ca Xyn30A benefits from five xylose-binding subsites which extend from the ?3 subsite to the +2 subsite of the binding cleft. These studies indicate that Ca Xyn30A is a GlcA- in dependent endoxylanase that may have evolved for the preferential recognition of α-1,2-Ara f substitutions on xylan chains.
机译:糖苷水解酶30亚家族8(GH30-8)β-1,4-内氧基酶是已知的,其依赖性依赖性函数需要识别血糖氧基氧基常见的α-1,2-连接的葡糖醛酸(GLCA)进行水解。结构研究表明,血糖醛氧基的GLCA部分通过六个氢键和盐桥配位。这些GLCA依赖性内唑基酶对不承受GLCA取代的Xylans具有显着的活性,例如未取代的线性木糖糖醇或谷物麸皮羰基体。在本研究中,我们介绍了来自醋酸梭菌(Ca Xyn30A)的木聚糖酶30A的结构和生化特征,其最初选择用于研究,这是由于GLCA协调环内的预测结构差异的研究。氨基酸序列比较表明,该革兰氏阳性衍生GH30-8更类似于革兰氏阴性衍生这些木聚糖内切的形式:在CA Xyn30A催化结构域(钙Xyn30A-CD)的发达的晶体结构模型的证实的假设。钙Xyn30A-CD水解木聚糖以显示最大速率与所述高度阿拉伯呋喃糖(ARA F)取代的阿拉伯木聚糖谷物线性和取代oligoxylosides。 Ca Xyn30A-CD水解大于木质糖大的木龙核苷酸,并显示出含有α-1,2-连接阿拉伯硫脲取代的木瓜糖苷的水解率增加。生物化学分析证实Ca Xyn30a受益于五个木糖结合底座,其从α3底座延伸到结合裂缝的+2个套房。这些研究表明,Ca Xyn30a是依赖于内氧基酶的Glca-,其可能已经进化为α-1,2-ARA F替代在Xylan链上的α-1,2-ARA F替代。

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  • 来源
    《The Biochemical Journal》 |2018年第9期|共19页
  • 作者单位

    Institute for Microbial and Biochemical Technology Forest Products Laboratory USDA Forest Service Madison WI U.S.A.;

    Institute for Microbial and Biochemical Technology Forest Products Laboratory USDA Forest Service Madison WI U.S.A.;

    Institute for Microbial and Biochemical Technology Forest Products Laboratory USDA Forest Service Madison WI U.S.A.;

    Institute for Microbial and Biochemical Technology Forest Products Laboratory USDA Forest Service Madison WI U.S.A.;

    Department of Pharmaceutical Sciences University of Maryland School of Pharmacy Baltimore MD U.S.A.;

    Institute for Bioscience and Biotechnology Research Department of Biochemistry and Molecular Biology University of Maryland School of Medicine Rockville MD U.S.A.;

    Department of Chemistry Physics and Geology Winthrop University Rock Hill SC U.S.A.;

    Department of Chemistry Physics and Geology Winthrop University Rock Hill SC U.S.A.;

    Department of Chemistry Physics and Geology Winthrop University Rock Hill SC U.S.A.;

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  • 原文格式 PDF
  • 正文语种 other
  • 中图分类 生物化学;
  • 关键词

    arabinoxylan; GH30; glycoside hydrolase family 30; protein structure; structure–function;

    机译:Arabinoxylan;GH30;糖苷水解酶30;蛋白质结构;结构功能;

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