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Convergent evolution sheds light on the anti-β-elimination mechanism common to family 1 and 10 polysaccharide lyases

机译:趋同进化揭示了家族1和10多糖裂解酶共有的抗β-消除机制

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摘要

Enzyme-catalyzed β-elimination of sugar uronic acids, exemplified by the degradation of plant cell wall pectins, plays an important role in a wide spectrum of biological processes ranging from the recycling of plant biomass through to pathogen virulence. The three-dimensional crystal structure of the catalytic module of a “family PL-10” polysaccharide lyase, Pel10Acm from Cellvibrio japonicus, solved at a resolution of 1.3 Å, reveals a new polysaccharide lyase fold and is the first example of a polygalacturonic acid lyase that does not exhibit the “parallel β-helix” topology. The “Michaelis” complex of an inactive mutant in association with the substrate trigalacturonate/Ca2+ reveals the catalytic machinery harnessed by this polygalacturonate lyase, which displays a stunning resemblance, presumably through convergent evolution, to the tetragalacturonic acid complex observed for a structurally unrelated polygalacturonate lyase from family PL-1. Common coordination of the −1 and +1 subsite saccharide carboxylate groups by a protein-liganded Ca2+ ion, the positioning of an arginine catalytic base in close proximity to the α-carbon hydrogen and numerous other conserved enzyme–substrate interactions, considered in light of mutagenesis data for both families, suggest a generic polysaccharide anti-β-elimination mechanism.
机译:糖醛糖酸的酶催化β-消除作用,以植物细胞壁果胶的降解为例,在从植物生物质的回收到病原体毒力的广泛的生物过程中都发挥着重要作用。 “家庭PL-10”多糖裂解酶,来自Cellvibrio japonicus的Pel10Acm的催化模块的三维晶体结构,以1.3 1.3的分辨率解析,揭示了一种新的多糖裂解酶折叠,是聚半乳糖醛酸裂解酶的第一个实例不会表现出“平行β螺旋”拓扑。失活突变体的“ Michaelis”复合物与底物半乳糖醛酸/ Ca 2+结合,揭示了这种多半乳糖醛酸裂合酶所利用的催化机制,推测是通过会聚进化,与在结构上不相关的多半乳糖醛酸裂合酶所观察到的四半乳糖醛酸复合物具有惊人的相似性。来自PL-1家庭。结合蛋白质的Ca2 +离子对-1和+1亚位糖基羧酸酯基团的共同配位,精氨酸催化碱基的位置紧靠α-碳氢以及许多其他保守的酶-底物相互作用,考虑到这两个家族的诱变数据表明,一种通用的多糖抗β-消除机制。

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