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Promiscuity in ligand-binding: The three-dimensional structure of a Piromyces carbohydrate-binding module, CBM29-2, in complex with cello- and mannohexaose

机译:配体结合中的混杂:Piromyces碳水化合物结合模块CBM29-2的三维结构,与纤维素和甘露糖糖复合

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摘要

Carbohydrate–protein recognition is central to many biological processes. Enzymes that act on polysaccharide substrates frequently contain noncatalytic domains, “carbohydrate-binding modules” (CBMs), that target the enzyme to the appropriate substrate. CBMs that recognize specific plant structural polysaccharides are often able to accommodate both the variable backbone and the side-chain decorations of heterogeneous ligands. “CBM29” modules, derived from a noncatalytic component of the Piromyces equi cellulase/hemicellulase complex, provide an example of this selective yet flexible recognition. They discriminate strongly against some polysaccharides while remaining relatively promiscuous toward both β-1,4-linked manno- and cello-oligosaccharides. This feature may reflect preferential, but flexible, targeting toward glucomannans in the plant cell wall. The three-dimensional structure of CBM29-2 and its complexes with cello- and mannohexaose reveal a β-jelly-roll topology, with an extended binding groove on the concave surface. The orientation of the aromatic residues complements the conformation of the target sugar polymer while accommodation of both manno- and gluco-configured oligo- and polysaccharides is conferred by virtue of the plasticity of the direct interactions from their axial and equatorial 2-hydroxyls, respectively. Such flexible ligand recognition targets the anaerobic fungal complex to a range of different components in the plant cell wall and thus plays a pivotal role in the highly efficient degradation of this composite structure by the microbial eukaryote.
机译:碳水化合物-蛋白质识别对于许多生物过程至关重要。作用于多糖底物上的酶通常包含非催化结构域,即“碳水化合物结合模块”(CBM),将酶靶向到适当的底物上。识别特定植物结构多糖的CBM通常能够容纳异质配体的可变主链和侧链修饰。源自Piromyces equi纤维素酶/半纤维素酶复合物的非催化成分的“ CBM29”模块提供了这种选择性而灵活的识别方法的示例。它们强烈区分某些多糖,而对β-1,4-连接的甘露寡糖和纤维寡糖相对混杂。此功能可能反映了针对植物细胞壁中的葡甘露聚糖的优先但灵活的目标。 CBM29-2的三维结构及其与纤维六糖和甘露糖六糖的复合物显示出β-果冻卷拓扑结构,在凹面具有延伸的结合槽。芳香族残基的取向补充了目标糖聚合物的构象,而甘露糖和葡萄糖配置的寡糖和多糖的容纳分别通过其轴向和赤道的2-羟基的直接相互作用的可塑性来实现。这种灵活的配体识别将厌氧真菌复合物靶向植物细胞壁中的一系列不同成分,因此在微生物真核生物对该复合结构的高效降解中起着关键作用。

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