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在重组鼠伤寒沙门氏菌中构建一条新型的不依赖丙酸盐途径用于生产聚(3-羟基丁酸酯-co-3-羟基戊酸酯)的代谢工程。

Metabolic engineering of a novel propionate-independent pathway for the production of poly(3-hydroxybutyrate-co-3-hydroxyvalerate) in recombinant Salmonella enterica serovar typhimurium.

作者信息

Aldor Ilana S, Kim Seon-Won, Prather Kristala L Jones, Keasling Jay D

机构信息

Department of Chemical Engineering, University of California, Berkeley, California 94720-1462, USA.

出版信息

Appl Environ Microbiol. 2002 Aug;68(8):3848-54. doi: 10.1128/AEM.68.8.3848-3854.2002.

Abstract

A pathway was metabolically engineered to produce poly(3-hydroxybutyrate-co-3-hydroxyvalerate) (PHBV), a biodegradable thermoplastic with proven commercial applications, from a single, unrelated carbon source. An expression system was developed in which a prpC strain of Salmonella enterica serovar Typhimurium, with a mutation in the ability to metabolize propionyl coenzyme A (propionyl-CoA), served as the host for a plasmid harboring the Acinetobacter polyhydroxyalkanoate synthesis operon (phaBCA) and a second plasmid with the Escherichia coli sbm and ygfG genes under an independent promoter. The sbm and ygfG genes encode a novel (2R)-methylmalonyl-CoA mutase and a (2R)-methylmalonyl-CoA decarboxylase, respectively, which convert succinyl-CoA, derived from the tricarboxylic acid cycle, to propionyl-CoA, an essential precursor of 3-hydroxyvalerate (HV). The S. enterica system accumulated PHBV with significant HV incorporation when the organism was grown aerobically with glycerol as the sole carbon source. It was possible to vary the average HV fraction in the copolymer by adjusting the arabinose or cyanocobalamin (precursor of coenzyme B12) concentration in the medium.

摘要

构建了一条代谢途径,可从单一的、不相关的碳源生产聚(3-羟基丁酸酯-co-3-羟基戊酸酯)(PHBV),这是一种具有已证实商业应用的可生物降解热塑性塑料。开发了一种表达系统,其中鼠伤寒沙门氏菌血清型鼠伤寒的prpC菌株,其代谢丙酰辅酶A(丙酰-CoA)的能力发生突变,用作携带不动杆菌聚羟基链烷酸酯合成操纵子(phaBCA)的质粒和在独立启动子下带有大肠杆菌sbm和ygfG基因的第二个质粒的宿主。sbm和ygfG基因分别编码一种新型的(2R)-甲基丙二酰-CoA变位酶和一种(2R)-甲基丙二酰-CoA脱羧酶,它们将三羧酸循环衍生的琥珀酰-CoA转化为丙酰-CoA,这是3-羟基戊酸酯(HV)的必需前体。当该生物体以甘油作为唯一碳源进行有氧生长时,鼠伤寒沙门氏菌系统积累了大量掺入HV的PHBV。通过调节培养基中的阿拉伯糖或氰钴胺素(辅酶B12的前体)浓度,可以改变共聚物中的平均HV含量。

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