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人几丁质酶催化壳聚糖水解。

Human chitotriosidase-catalyzed hydrolysis of chitosan.

机构信息

Department of Chemistry, Biotechnology and Food Science, Norwegian University of Life Sciences, N-1432 Ås, Norway.

出版信息

Biochemistry. 2012 Jan 10;51(1):487-95. doi: 10.1021/bi2015585. Epub 2011 Dec 20.

Abstract

Chitotriosidase (HCHT) is one of two family 18 chitinases produced by humans, the other being acidic mammalian chitinase (AMCase). The enzyme is thought to be part of the human defense mechanism against fungal parasites, but its precise role and the details of its enzymatic properties have not yet been fully unraveled. We have studied the properties of HCHT by analyzing how the enzyme acts on high-molecular weight chitosans, soluble copolymers of β-1,4-linked N-acetylglucosamine (GlcNAc, A), and glucosamine (GlcN, D). Using methods for in-depth studies of the chitinolytic machinery of bacterial family 18 enzymes, we show that HCHT degrades chitosan primarily via an endoprocessive mechanism, as would be expected on the basis of the structural features of its substrate-binding cleft. The preferences of HCHT subsites for acetylated versus nonacetylated sugars were assessed by sequence analysis of obtained oligomeric products showing a very strong, absolute, and a relative weak preference for an acetylated unit in the -2, -1, and +1 subsites, respectively. The latter information is important for the design of inhibitors that are specific for the human chitinases and also provides insight into what kind of products may be formed in vivo upon administration of chitosan-containing medicines or food products.

摘要

几丁质酶 3(HCHT)是人类产生的两种家族 18 几丁质酶之一,另一种是酸性哺乳动物几丁质酶(AMCase)。该酶被认为是人体抵御真菌寄生虫的防御机制的一部分,但它的确切作用及其酶学特性的细节尚未完全阐明。我们通过分析该酶对高分子量壳聚糖的作用,研究了 HCHT 的特性,壳聚糖是β-1,4 连接的 N-乙酰葡萄糖胺(GlcNAc,A)和葡萄糖胺(GlcN,D)的可溶性共聚物。使用深入研究细菌家族 18 酶的甲壳质酶机制的方法,我们表明 HCHT 主要通过内过程机制降解壳聚糖,这基于其底物结合裂隙的结构特征。通过对获得的低聚物产物进行序列分析,评估了 HCHT 亚基对乙酰化与非乙酰化糖的偏好性,结果显示在-2、-1 和+1 亚基中,对乙酰化单元具有非常强、绝对和相对弱的偏好性。后者的信息对于设计特异性针对人类几丁质酶的抑制剂非常重要,并且还提供了有关在给予含有壳聚糖的药物或食品产品时体内可能形成何种产物的信息。

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