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谷氨酸棒杆菌柠檬酸循环中膜结合型和胞质型苹果酸脱氢酶的功能。

Functions of the membrane-associated and cytoplasmic malate dehydrogenases in the citric acid cycle of Corynebacterium glutamicum.

作者信息

Molenaar D, van der Rest M E, Drysch A, Yücel R

机构信息

Biotechnologisches Zentrallabor, Geb. 25.12, Heinrich-Heine-Universität, D-40225 Düsseldorf, Germany.

出版信息

J Bacteriol. 2000 Dec;182(24):6884-91. doi: 10.1128/JB.182.24.6884-6891.2000.

Abstract

Like many other bacteria, Corynebacterium glutamicum possesses two types of L-malate dehydrogenase, a membrane-associated malate:quinone oxidoreductase (MQO; EC 1.1.99.16) and a cytoplasmic malate dehydrogenase (MDH; EC 1.1.1.37) The regulation of MDH and of the three membrane-associated dehydrogenases MQO, succinate dehydrogenase (SDH), and NADH dehydrogenase was investigated. MQO, MDH, and SDH activities are regulated coordinately in response to the carbon and energy source for growth. Compared to growth on glucose, these activities are increased during growth on lactate, pyruvate, or acetate, substrates which require high citric acid cycle activity to sustain growth. The simultaneous presence of high activities of both malate dehydrogenases is puzzling. MQO is the most important malate dehydrogenase in the physiology of C. glutamicum. A mutant with a site-directed deletion in the mqo gene does not grow on minimal medium. Growth can be partially restored in this mutant by addition of the vitamin nicotinamide. In contrast, a double mutant lacking MQO and MDH does not grow even in the presence of nicotinamide. Apparently, MDH is able to take over the function of MQO in an mqo mutant, but this requires the presence of nicotinamide in the growth medium. It is shown that addition of nicotinamide leads to a higher intracellular pyridine nucleotide concentration, which probably enables MDH to catalyze malate oxidation. Purified MDH from C. glutamicum catalyzes oxaloacetate reduction much more readily than malate oxidation at physiological pH. In a reconstituted system with isolated membranes and purified MDH, MQO and MDH catalyze the cyclic conversion of malate and oxaloacetate, leading to a net oxidation of NADH. Evidence is presented that this cyclic reaction also takes place in vivo. As yet, no phenotype of an mdh deletion alone was observed, which leaves a physiological function for MDH in C. glutamicum obscure.

摘要

与许多其他细菌一样,谷氨酸棒杆菌拥有两种类型的L-苹果酸脱氢酶,一种是膜相关的苹果酸:醌氧化还原酶(MQO;EC 1.1.99.16)和一种细胞质苹果酸脱氢酶(MDH;EC 1.1.1.37)。研究了MDH以及三种膜相关脱氢酶MQO、琥珀酸脱氢酶(SDH)和NADH脱氢酶的调控。MQO、MDH和SDH的活性根据生长的碳源和能源进行协调调控。与在葡萄糖上生长相比,在乳酸、丙酮酸或乙酸上生长时,这些活性会增加,这些底物需要高柠檬酸循环活性来维持生长。两种苹果酸脱氢酶同时具有高活性令人费解。MQO是谷氨酸棒杆菌生理学中最重要的苹果酸脱氢酶。在mqo基因中进行定点缺失的突变体在基本培养基上无法生长。通过添加维生素烟酰胺,该突变体的生长可以部分恢复。相比之下,缺乏MQO和MDH的双突变体即使在有烟酰胺的情况下也无法生长。显然,MDH能够在mqo突变体中接管MQO的功能,但这需要在生长培养基中存在烟酰胺。结果表明,添加烟酰胺会导致细胞内吡啶核苷酸浓度升高,这可能使MDH能够催化苹果酸氧化。在生理pH值下,从谷氨酸棒杆菌纯化的MDH催化草酰乙酸还原比催化苹果酸氧化更容易。在一个由分离的膜和纯化的MDH组成的重构系统中,MQO和MDH催化苹果酸和草酰乙酸的循环转化,导致NADH的净氧化。有证据表明这种循环反应在体内也会发生。到目前为止,尚未观察到单独缺失mdh的表型,这使得谷氨酸棒杆菌中MDH的生理功能仍不清楚。

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