Jitrapakdee S, Wallace J C
Department of Biochemistry, University of Adelaide, Adelaide, South Australia 5005, Australia.
Biochem J. 1999 May 15;340 ( Pt 1)(Pt 1):1-16. doi: 10.1042/bj3400001.
Pyruvate carboxylase (PC; EC 6.4.1.1), a member of the biotin-dependent enzyme family, catalyses the ATP-dependent carboxylation of pyruvate to oxaloacetate. PC has been found in a wide variety of prokaryotes and eukaryotes. In mammals, PC plays a crucial role in gluconeogenesis and lipogenesis, in the biosynthesis of neurotransmitter substances, and in glucose-induced insulin secretion by pancreatic islets. The reaction catalysed by PC and the physical properties of the enzyme have been studied extensively. Although no high-resolution three-dimensional structure has yet been determined by X-ray crystallography, structural studies of PC have been conducted by electron microscopy, by limited proteolysis, and by cloning and sequencing of genes and cDNA encoding the enzyme. Most well characterized forms of active PC consist of four identical subunits arranged in a tetrahedron-like structure. Each subunit contains three functional domains: the biotin carboxylation domain, the transcarboxylation domain and the biotin carboxyl carrier domain. Different physiological conditions, including diabetes, hyperthyroidism, genetic obesity and postnatal development, increase the level of PC expression through transcriptional and translational mechanisms, whereas insulin inhibits PC expression. Glucocorticoids, glucagon and catecholamines cause an increase in PC activity or in the rate of pyruvate carboxylation in the short term. Molecular defects of PC in humans have recently been associated with four point mutations within the structural region of the PC gene, namely Val145-->Ala, Arg451-->Cys, Ala610-->Thr and Met743-->Thr.
丙酮酸羧化酶(PC;EC 6.4.1.1)是生物素依赖性酶家族的成员,催化丙酮酸依赖ATP羧化为草酰乙酸。PC已在多种原核生物和真核生物中被发现。在哺乳动物中,PC在糖异生和脂肪生成、神经递质物质的生物合成以及胰岛的葡萄糖诱导胰岛素分泌中起关键作用。PC催化的反应以及该酶的物理性质已得到广泛研究。尽管尚未通过X射线晶体学确定其高分辨率三维结构,但已通过电子显微镜、有限蛋白酶解以及对编码该酶的基因和cDNA进行克隆和测序对PC进行了结构研究。大多数已充分表征的活性PC形式由四个相同的亚基组成,排列成四面体状结构。每个亚基包含三个功能域:生物素羧化域、转羧化域和生物素羧基载体域。不同的生理状况,包括糖尿病、甲状腺功能亢进、遗传性肥胖和出生后发育,通过转录和翻译机制增加PC的表达水平,而胰岛素则抑制PC的表达。糖皮质激素、胰高血糖素和儿茶酚胺在短期内会导致PC活性或丙酮酸羧化速率增加。人类PC的分子缺陷最近与PC基因结构区域内的四个点突变有关,即Val145→Ala、Arg451→Cys、Ala610→Thr和Met743→Thr。