牛肝谷氨酸脱氢酶的产物抑制研究。

A product-inhibition study of bovine liver glutamate dehydrogenase.

作者信息

Engel P C, Chen S S

出版信息

Biochem J. 1975 Nov;151(2):305-18. doi: 10.1042/bj1510305.

DOI:10.1042/bj1510305

PMID:175778

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1172361/

Abstract

Initial rates of oxidative deamination of L-glutamate with NAD+ as coenzyme, and of reductive aminiation of 2-oxoglutarate with NADH as coenzyme, catalysed by bovine liver glutamate dehydrogenase were measured in 0.111 M-sodium phosphate buffer, pH 7, at 25 degrees C, in the absence and presence of product inhibitors. All 12 possible combinations of variable substrate and product inhibitor were used. 2. Strict competition was observed between NAD+ and NADH, and between glutamate and 2-oxoglutarate. All other inhibition patterns were clearly non-competitive, except for inhibition by NH4+ with NAD+ as variable substrate. Here the extrapolation did not permit a clear distinction between competitive and non-competitive inhibition. 3. Mutually non-competitive behaviour between glutamate and NH4+ indicates that these substrates can be bound at the active site simultaneously. 4. Primary Lineweaver-Burk plots and derived secondary plots of slopes and intercepts against inhibitor concentration were linear, with one exception: with 2-oxoglutarate as variable substrate, the replot of primary intercepts against inhibitory NAD+ concentration was curved. 5. Separate Ki values were evaluated for the effect of each product inhibitor on the individual terms in the reciprocal initial-rate equations. With this information it is possible to calculate rates for any combination of substrate concentrations within the experimental range with any concentration of a single product inhibitor. 6. The inhibition patterns are consistent with neither a simple compulsory-order mechanism nor a rapid-equilibrium random-order mechanism without modification. They can, however, be reconciled with either type of mechanism by postulating appropirate abortive complexes. Of the two compulsory sequences that have been proposed, one, that in which the order of binding is NADH, NH4+, 2-oxoglutarate, requires an implausible pattern of abortive complex-formation to account for the results. 7. On the basis of a rapid-equilibrium random-order mechanism, dissociation constants can be calculated from the Ki values. Where these can be compared with independent estimates from the kinetics of the uninhibited reaction or from direct measurements of substrate binding, the agreement is reasonable good. On balance, therefore, the results provide further support for the rapid-equilibrium random-order mechanism under these conditions.

摘要

在0.111M磷酸钠缓冲液（pH7）中，于25℃，在不存在和存在产物抑制剂的情况下，测定了牛肝谷氨酸脱氢酶催化的以NAD⁺为辅酶的L-谷氨酸氧化脱氨的初始速率，以及以NADH为辅酶的2-氧代戊二酸还原胺化的初始速率。使用了可变底物和产物抑制剂的所有12种可能组合。2. 观察到NAD⁺与NADH之间以及谷氨酸与2-氧代戊二酸之间存在严格竞争。除了以NAD⁺作为可变底物时NH₄⁺的抑制作用外，所有其他抑制模式均明显为非竞争性。在此，外推法无法明确区分竞争性抑制和非竞争性抑制。3. 谷氨酸与NH₄⁺之间的相互非竞争性行为表明这些底物可同时结合在活性位点。4. 初级Lineweaver-Burk图以及推导的斜率和截距相对于抑制剂浓度的二级图是线性的，但有一个例外：以2-氧代戊二酸作为可变底物时，初级截距相对于抑制性NAD⁺浓度的重绘图是弯曲的。5. 针对每种产物抑制剂对倒数初始速率方程中各个项的影响评估了单独的Ki值。利用这些信息，可以计算在实验范围内任何底物浓度组合与任何单一产物抑制剂浓度下的速率。6. 这些抑制模式既不符合简单的强制顺序机制，也不符合未经修改的快速平衡随机顺序机制。然而，通过假设适当的无效复合物，可以使它们与任何一种机制相协调。在已提出的两种强制顺序中，一种是结合顺序为NADH、NH₄⁺、2-氧代戊二酸，为了解释结果需要一种不合理的无效复合物形成模式。7. 基于快速平衡随机顺序机制，可以从Ki值计算解离常数。在可以将这些值与来自无抑制反应动力学的独立估计值或底物结合的直接测量值进行比较的情况下，一致性相当好。因此，总的来说，这些结果为这些条件下的快速平衡随机顺序机制提供了进一步的支持。