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首页> 外文期刊>Acta crystallographica. Section D, Structural biology. >Three-dimensional structures of two heavily N-glycosylated Aspergillus sp family GH3 beta-D-glucosidases
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Three-dimensional structures of two heavily N-glycosylated Aspergillus sp family GH3 beta-D-glucosidases

机译:两个严重的三维结构家庭GH3 N-glycosylated曲霉菌spbeta-D-glucosidases

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The industrial conversion of cellulosic plant biomass into useful products such as biofuels is a major societal goal. These technologies harness diverse plant degrading enzymes, classical exo- and endo-acting cellulases and, increasingly, cellulose-active lytic polysaccharide monooxygenases, to deconstruct the recalcitrant beta-D-linked polysaccharide. A major drawback with this process is that the exo-acting cellobiohydrolases suffer from severe inhibition from their cellobiose product. beta-D-Glucosidases are therefore important for liberating glucose from cellobiose and thereby relieving limiting product inhibition. Here, the three-dimensional structures of two industrially important family GH3 beta-D-glucosidases from Aspergillus fumigatus and A. oryzae, solved by molecular replacement and refined at 1.95 angstrom resolution, are reported. Both enzymes, which share 78% sequence identity, display a three-domain structure with the catalytic domain at the interface, as originally shown for barley beta-D-glucan exohydrolase, the first three-dimensional structure solved from glycoside hydrolase family GH3. Both enzymes show extensive N-glycosylation, with only a few external sites being truncated to a single GlcNAc molecule. Those glycans N-linked to the core of the structure are identified purely as high-mannose trees, and establish multiple hydrogen bonds between their sugar components and adjacent protein side chains. The extensive glycans pose special problems for crystallographic refinement, and new techniques and protocols were developed especially for this work. These protocols ensured that all of the d-pyranosides in the glycosylation trees were modelled in the preferred minimum-energy C-4(1) chair conformation and should be of general application to refinements of other crystal structures containing O- or N-glycosylation. The Aspergillus GH3 structures, in light of other recent three-dimensional structures, provide insight into fungal beta-D-glucosidases and provide a platform on which to inform and inspire new generations of variant enzymes for industrial application.
机译:工业转化纤维素的植物生物质转化成有用的产品,如生物燃料一个重大的社会目标。不同植物降解酶,古典外endo-acting了多种纤维素酶和越来越多的cellulose-active溶解多糖单氧酶,顽固的解构beta-D-linked多糖。在这一过程中exo-actingcellobiohydrolases受到严重的抑制从他们的纤维二糖的产品。beta-D-Glucosidases因此重要从而解放从纤维二糖和葡萄糖解除限制产物抑制。两个工业的三维结构重要的家庭GH3 beta-D-glucosidases来自烟曲霉菌和a . oryzae解决分子置换和精制为1.95埃分辨率,报告。分享78%序列的身份,显示一个吗物种三域分类与催化结构域接口,为大麦最初显示beta-D-glucan exohydrolase,第一从配糖体三维结构解决水解酶家族GH3。N-glycosylation,只有一些外部网站一个GlcNAc分子被截断。这些聚糖N-linked的核心结构确定high-mannose纯粹树,建立多个氢键在糖组件和相邻蛋白质侧链。特殊问题结晶细化,开发和新技术和协议特别是对于这项工作。所有的d-pyranosides糖基化树被模仿喜欢所以c - 4(1)椅子构象,应该通用应用程序其他的晶体结构的改进含O或N-glycosylation。GH3结构,根据最近其他三维结构,提供洞察力为真菌beta-D-glucosidases和提供通知和激发新平台一代又一代的变异酶工业应用程序。

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