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糖原:生物合成与调控

Glycogen: Biosynthesis and Regulation.

作者信息

Preiss Jack

出版信息

EcoSal Plus. 2009 Aug;3(2). doi: 10.1128/ecosalplus.4.7.4.

Abstract

The accumulation of glycogen occurs in Escherichia coli and Salmonella enterica serovar Typhimurium as well as in many other bacteria. Glycogen will be formed when there is an excess of carbon under conditions in which growth is limited due to the lack of a growth nutrient, e.g., a nitrogen source. The structural genes of the glycogen biosynthetic enzymes of E. coli and S. serovar Typhimurium have been cloned previously, and that has provided insights in the genetic regulation of glycogen synthesis. An important aspect of the regulation of glycogen synthesis is the allosteric regulation of the ADP-Glc PPase. The current information, views, and concepts regarding the regulation of enzyme activity and the expression of the glycogen biosynthetic enzymes are presented in this review. The recent information on the amino acid residues critical for the activity of both glycogen synthase and branching enzyme (BE) is also presented. The residue involved in catalysis in the E. coli ADP-Glc PPase was determined by comparing a predicted structure of the enzyme with the known three-dimensional structures of sugar-nucleotide PPase domains. The molecular cloning of the E. coliglg K-12 structural genes greatly facilitated the subsequent study of the genetic regulation of bacterial glycogen biosynthesis. Results from studies of glycogen excess E. coli B mutants SG3 and AC70R1, which exhibit enhanced levels of the enzymes in the glycogen synthesis pathway (i.e., they are derepressed mutants), suggested that glycogen synthesis is under negative genetic regulation.

摘要

糖原的积累发生在大肠杆菌、鼠伤寒沙门氏菌以及许多其他细菌中。当由于缺乏生长营养物质(如氮源)导致生长受限的情况下,若存在过量碳源,糖原就会形成。大肠杆菌和鼠伤寒沙门氏菌糖原生物合成酶的结构基因此前已被克隆,这为糖原合成的遗传调控提供了见解。糖原合成调控的一个重要方面是ADP - 葡萄糖焦磷酸化酶的变构调节。本综述介绍了有关酶活性调节和糖原生物合成酶表达的当前信息、观点和概念。还介绍了最近关于对糖原合酶和分支酶(BE)活性至关重要的氨基酸残基的信息。通过将该酶的预测结构与糖核苷酸焦磷酸化酶结构域的已知三维结构进行比较,确定了大肠杆菌ADP - 葡萄糖焦磷酸化酶中参与催化的残基。大肠杆菌K - 12结构基因的分子克隆极大地促进了随后对细菌糖原生物合成遗传调控的研究。对糖原过量的大肠杆菌B突变体SG3和AC70R1的研究结果表明,糖原合成处于负遗传调控之下,这两种突变体在糖原合成途径中酶的水平有所提高(即它们是去阻遏突变体)。

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