Pettersson H, Olsson P, Bülow L, Pettersson G
Avdelningen für Biokemi and Avdelningen für Tillämpad Biokemi, Kemicentrum, Lunds Universitet, Lund, Sweden.
Eur J Biochem. 2000 Aug;267(16):5041-6. doi: 10.1046/j.1432-1327.2000.01558.x.
The mechanistic implications of the kinetic behaviour of a fusion protein of mitochondrial malate dehydrogenase and citrate synthase have been reanalysed in view of predictions based on experimentally determined kinetic parameter values for the dehydrogenase and synthase activities of the protein. The results show that the time-course of citrate formation from malate in the coupled reaction catalysed by the fusion protein can be most satisfactorily accounted for in terms of a free-diffusion mechanism when consideration is taken to the inhibitory effects of NADH and oxaloacetate on the malate dehydrogenase activity. The effect of aspartate aminotransferase on the coupled reaction is likewise fully consistent with that expected for a free-diffusion mechanism. It is concluded that no tenable kinetic evidence is available to support the proposal that the fusion protein catalyses citrate formation from malate by a mechanism involving channelling of the intermediate oxaloacetate.
基于对该蛋白质中苹果酸脱氢酶和柠檬酸合酶活性的实验测定动力学参数值所做的预测,对线粒体苹果酸脱氢酶与柠檬酸合酶融合蛋白的动力学行为的机制含义进行了重新分析。结果表明,当考虑到NADH和草酰乙酸对苹果酸脱氢酶活性的抑制作用时,融合蛋白催化的偶联反应中从苹果酸形成柠檬酸的时间进程可以用自由扩散机制最令人满意地解释。天冬氨酸转氨酶对偶联反应的影响同样与自由扩散机制所预期的完全一致。得出的结论是,没有可靠的动力学证据支持融合蛋白通过涉及中间产物草酰乙酸通道化的机制催化从苹果酸形成柠檬酸这一观点。