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多糖降解酶的结构与功能比较

Structural and functional comparison of polysaccharide-degrading enzymes.

作者信息

Jedrzejas M J

机构信息

Department of Microbiology, University of Alabama at Birmingham, 35294-2041, USA.

出版信息

Crit Rev Biochem Mol Biol. 2000;35(3):221-51. doi: 10.1080/10409230091169195.

Abstract

Sugar molecules as well as enzymes degrading them are ubiquitously present in physiological systems, especially for vertebrates. Polysaccharides have at least two aspects to their function, one due to their mechanical properties and the second one involves multiple regulatory processes or interactions between molecules, cells, or extracellular space. Various bacteria exert exogenous pressures on their host organism to diversity glycans and their structures in order for the host organism to evade the destructive function of such microbes. Many bacterial organism produce glycan-degrading enzymes in order to facilitate their invasion of host tissues. Such polysaccharide degrading enzymes utilize mainly two modes of polysaccharide-degradation, a hydrolysis and a beta-elimination process. The three-dimensional structures of several of these enzymes have been elucidated recently using X-ray crystallography. There are many common structural motifs among these enzymes, mainly the presence of an elongated cleft transversing these molecules which functions as a polysaccharide substrate binding site as well as the catalytic site for these enzymes. The detailed structural information obtained about these enzymes allowed formulation of proposed mechanisms of their action. The polysaccharide lyases utilize a proton acceptance and donation mechanism (PAD), whereas polysaccharide hydrolases use a direct double displacement (DD) mechanism to degrade their substrates.

摘要

糖分子以及降解它们的酶普遍存在于生理系统中,尤其是在脊椎动物体内。多糖的功能至少有两个方面,一方面归因于其机械性能,另一方面涉及分子、细胞或细胞外空间之间的多种调节过程或相互作用。各种细菌对其宿主生物体施加外部压力,促使聚糖及其结构多样化,以便宿主生物体规避此类微生物的破坏功能。许多细菌生物体产生聚糖降解酶,以促进它们对宿主组织的侵袭。此类多糖降解酶主要利用两种多糖降解模式,即水解和β-消除过程。最近利用X射线晶体学阐明了其中几种酶的三维结构。这些酶之间有许多共同的结构基序,主要是存在一条贯穿这些分子的细长裂缝,它充当多糖底物结合位点以及这些酶的催化位点。所获得的关于这些酶的详细结构信息有助于阐述其作用机制。多糖裂解酶利用质子接受和供体机制(PAD),而多糖水解酶则使用直接双置换(DD)机制来降解其底物。

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