Agrawal Nitish, Hong Baoyu, Mihai Cornelia, Kohen Amnon
Department of Chemistry, University of Iowa, Iowa City, Iowa 52242, USA.
Biochemistry. 2004 Feb 24;43(7):1998-2006. doi: 10.1021/bi036124g.
The enzyme thymidylate synthase (TS) catalyzes a complex reaction that involves forming and breaking at least six covalent bonds. The physical nature of the hydride transfer step in this complex reaction cascade has been studied by means of isotope effects and their temperature dependence. Competitive kinetic isotope effects (KIEs) on the second-order rate constant (V/K) were measured over a temperature range of 5-45 degrees C. The observed H/T ((T)V/K(H)) and D/T ((T)V/K(D)) KIEs were used to calculate the intrinsic KIEs throughout the temperature range. The Swain-Schaad relationships between the H/T and D/T V/K KIEs revealed that the hydride transfer step is the rate-determining step at the physiological temperature of Escherichia coli (20-30 degrees C) but is only partly rate-determining at elevated and reduced temperatures. H/D KIE on the first-order rate constant k(cat) ((D)k = 3.72) has been previously reported [Spencer et al. (1997) Biochemistry 36, 4212-4222]. Additionally, the Swain-Schaad relationships between that (D)k and the V/K KIEs reported here suggested that at 20 degrees C the hydride transfer step is the rate-determining step for both rate constants. Intrinsic KIEs were calculated here and were found to be virtually temperature independent (DeltaE(a) = 0 within experimental error). The isotope effects on the preexponential Arrhenius factors for the intrinsic KIEs were A(H)/A(T) = 6.8 +/- 2.8 and A(D)/A(T) = 1.9 +/- 0.25. Both effects are significantly above the semiclassical (no-tunneling) predicted values and indicate a contribution of quantum mechanical tunneling to this hydride transfer reaction. Tunneling correction to transition state theory would predict that these isotope effects on activation parameters result from no energy of activation for all isotopes. Yet, initial velocity measurements over the same temperature range indicate cofactor inhibition and result in significant activation energy on k(cat) (4.0 +/- 0.1 kcal/mol). Taken together, the temperature-independent KIEs, the large isotope effects on the preexponential Arrhenius factors, and a significant energy of activation all suggest vibrationally enhanced hydride tunneling in the TS-catalyzed reaction.
胸苷酸合成酶(TS)催化的复杂反应涉及至少六个共价键的形成和断裂。通过同位素效应及其温度依赖性,对这一复杂反应级联中氢化物转移步骤的物理性质进行了研究。在5-45摄氏度的温度范围内,测量了对二级速率常数(V/K)的竞争动力学同位素效应(KIEs)。利用观察到的H/T((T)V/K(H))和D/T((T)V/K(D))KIEs计算了整个温度范围内的本征KIEs。H/T和D/T V/K KIEs之间的斯温-沙德关系表明,在大肠杆菌的生理温度(20-30摄氏度)下,氢化物转移步骤是速率决定步骤,但在升高和降低的温度下只是部分速率决定步骤。先前已报道了对一级速率常数k(cat)的H/D KIE((D)k = 3.72)[斯宾塞等人(1997年)《生物化学》36,4212-4222]。此外,此处报道的(D)k与V/K KIEs之间的斯温-沙德关系表明,在20摄氏度时,氢化物转移步骤对两个速率常数都是速率决定步骤。此处计算了本征KIEs,发现其实际上与温度无关(在实验误差范围内ΔE(a)=0)。本征KIEs的预指数阿仑尼乌斯因子的同位素效应为A(H)/A(T)=6.8±2.8和A(D)/A(T)=1.9±0.25。这两种效应都显著高于半经典(无隧穿)预测值,表明量子力学隧穿对该氢化物转移反应有贡献。对过渡态理论的隧穿校正将预测,这些对活化参数的同位素效应是由于所有同位素都没有活化能。然而,在相同温度范围内的初始速度测量表明存在辅因子抑制,并且导致k(cat)上有显著的活化能(4.0±0.1千卡/摩尔)。综上所述,与温度无关的KIEs、对预指数阿仑尼乌斯因子的大同位素效应以及显著的活化能都表明在TS催化的反应中存在振动增强的氢化物隧穿。
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