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首页> 外文期刊>Scientific reports. >Ligand-binding specificity and promiscuity of the main lignocellulolytic enzyme families as revealed by active-site architecture analysis
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Ligand-binding specificity and promiscuity of the main lignocellulolytic enzyme families as revealed by active-site architecture analysis

机译:活性位点结构分析揭示了主要木质纤维素分解酶家族的配体结合特异性和混杂性

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Biomass can be converted into sugars by a series of lignocellulolytic enzymes, which belong to the glycoside hydrolase (GH) families summarized in CAZy databases. Here, using a structural bioinformatics method, we analyzed the active site architecture of the main lignocellulolytic enzyme families. The aromatic amino acids Trp/Tyr and polar amino acids Glu/Asp/Asn/Gln/Arg occurred at higher frequencies in the active site architecture than in the whole enzyme structure. And the number of potential subsites was significantly different among different families. In the cellulase and xylanase families, the conserved amino acids in the active site architecture were mostly found at the -2 to +1 subsites, while in β-glucosidase they were mainly concentrated at the -1 subsite. Families with more conserved binding amino acid residues displayed strong selectivity for their ligands, while those with fewer conserved binding amino acid residues often exhibited promiscuity when recognizing ligands. Enzymes with different activities also tended to bind different hydroxyl oxygen atoms on the ligand. These results may help us to better understand the common and unique structural bases of enzyme-ligand recognition from different families and provide a theoretical basis for the functional evolution and rational design of major lignocellulolytic enzymes.
机译:可以通过一系列木质纤维素分解酶将生物质转化为糖,这些酶属于CAZy数据库中概括的糖苷水解酶(GH)家族。在这里,我们使用结构生物信息学方法,分析了主要木质纤维素分解酶家族的活性位点结构。芳香族氨基酸Trp / Tyr和极性氨基酸Glu / Asp / Asn / Gln / Arg在活性位点结构中的发生频率高于整个酶结构。不同家庭之间潜在子站点的数量也明显不同。在纤维素酶和木聚糖酶家族中,活性位点结构中的保守氨基酸主要存在于-2至+1个亚位点,而在β-葡萄糖苷酶中则主要集中于-1个亚位点。具有更保守的结合氨基酸残基的家族对它们的配体表现出强的选择性,而那些具有更少的保守结合氨基酸残基的家族在识别配体时常常表现出混杂。具有不同活性的酶也倾向于结合配体上的不同羟基氧原子。这些结果可能有助于我们更好地了解不同家族的酶-配体识别的共同和独特的结构基础,并为主要的木质纤维素分解酶的功能进化和合理设计提供理论依据。

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