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通过csrA基因对大肠杆菌中枢碳水化合物代谢的多效性调控

Pleiotropic regulation of central carbohydrate metabolism in Escherichia coli via the gene csrA.

作者信息

Sabnis N A, Yang H, Romeo T

机构信息

Department of Microbiology, University of North Texas Health Science Center at Fort Worth 76107-2699, USA.

出版信息

J Biol Chem. 1995 Dec 8;270(49):29096-104. doi: 10.1074/jbc.270.49.29096.

Abstract

The carbon storage regulator gene csrA has been shown previously to dramatically affect the biosynthesis of intracellular glycogen in Escherichia coli through its negative control of the expression of two glycogen biosynthetic operons and the gluconeogenic gene pckA (Romeo, T., Gong, M., Liu, M. Y., and Brun-Zinkernagel, A. M. (1993) J. Bacteriol. 175, 4744-4755). Examination of the effects of csrA on several enzymes, genes, and metabolites of central carbohydrate metabolism now establishes a more extensive role for csrA in directing intracellular carbon flux. Phosphoglucomutase and the gluconeogenic enzymes fructose-1,6-bisphosphatase and phosphoenolpyruvate synthetase were found to be under the negative control of csrA, and these enzyme activities were maximal during the early stationary phase of growth. The enzymes glucose-6-phosphate isomerase, triose-phosphate isomerase, and enolase were positively regulated by csrA. Thus, csrA exerts reciprocal effects on glycolysis versus gluconeogenesis and glycogen biosynthesis. The glycolytic isozymes pyruvate kinase F and A (encoded by pykF and pykA, respectively) and phosphofructokinase I and II (pfkA and pfkB, respectively) exhibited differential regulation via csrA. Since the individual members of these isozyme pairs are allosterically regulated by different cellular metabolites, csrA is also capable of fine-tuning the allosteric regulation of glycolysis. In contrast, the expression of genes of the pentose phosphate pathway was weakly or negligibly affected by csrA.

摘要

碳储存调节基因csrA先前已被证明通过对两个糖原生物合成操纵子和糖异生基因pckA表达的负调控,显著影响大肠杆菌细胞内糖原的生物合成(罗密欧,T.,龚,M.,刘,M.Y.,和布伦 - 津克纳格尔,A.M.(1993年)《细菌学杂志》175,4744 - 4755)。现在研究csrA对中心碳水化合物代谢的几种酶、基因和代谢物的影响,确定了csrA在指导细胞内碳通量方面发挥更广泛的作用。发现磷酸葡萄糖变位酶以及糖异生酶果糖 - 1,6 - 二磷酸酶和磷酸烯醇丙酮酸合成酶受csrA的负调控,并且这些酶活性在生长的早期稳定期最高。葡萄糖 - 6 - 磷酸异构酶、磷酸丙糖异构酶和烯醇酶受csrA的正调控。因此,csrA对糖酵解与糖异生及糖原生物合成发挥相反的作用。糖酵解同工酶丙酮酸激酶F和A(分别由pykF和pykA编码)以及磷酸果糖激酶I和II(分别为pfkA和pfkB)通过csrA表现出差异调节。由于这些同工酶对的各个成员受不同细胞代谢物的变构调节,csrA也能够微调糖酵解的变构调节。相比之下,磷酸戊糖途径基因的表达受csrA的影响较弱或可忽略不计。

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