Department of Biology, The Catholic University of America, Washington, DC 20064, USA.
Proc Natl Acad Sci U S A. 2012 Nov 6;109(45):18453-8. doi: 10.1073/pnas.1208771109. Epub 2012 Oct 24.
The thermodynamics of binding reactions is usually studied in the framework of the linear van't Hoff analysis of the temperature dependence of the equilibrium constant. The logarithm of the equilibrium constant is plotted versus inverse temperature to discriminate between two terms: an enthalpic contribution that is linear in the inverse temperature, and a temperature-independent entropic contribution. When we apply this approach to a particular case-blockage of the anthrax PA(63) channel by a multicharged cyclodextrin derivative-we obtain a nearly linear behavior with a slope that is characterized by enthalpy of about 1 kcal/mol. In contrast, from blocker partitioning between the channel and the bulk, we estimate the depth of the potential well for the blocker in the channel to be at least 8 kcal/mol. To understand this apparent discrepancy, we use a simple model of particle interaction with the channel and show that this significant difference between the two estimates is due to the temperature dependence of the physical forces between the blocker and the channel. In particular, we demonstrate that if the major component of blocker-channel interaction is van der Waals interactions and/or Coulomb forces in water, the van't Hoff enthalpy of the binding reaction may be close to zero or even negative, including cases of relatively strong binding. The results are quite general and, therefore, of importance for studies of enzymatic reactions, rational drug design, small-molecule binding to proteins, protein-protein interactions, and protein folding, among others.
结合反应的热力学通常在平衡常数的温度依赖性的线性范特霍夫分析的框架内进行研究。将平衡常数的对数相对于倒数温度作图,以区分两个术语:与倒数温度呈线性关系的焓贡献,以及与温度无关的熵贡献。当我们将这种方法应用于特定情况 - 多电荷环糊精衍生物阻塞炭疽杆菌 PA(63)通道时 - 我们得到了几乎线性的行为,斜率由约 1 kcal/mol 的焓来表征。相比之下,从通道和体相之间的阻断剂分配来看,我们估计阻断剂在通道中的势阱深度至少为 8 kcal/mol。为了理解这种明显的差异,我们使用了一个简单的粒子与通道相互作用模型,并表明这两个估计值之间的显著差异是由于阻断剂和通道之间的物理力随温度的变化。特别是,我们证明如果阻断剂-通道相互作用的主要成分是范德华相互作用和/或水中的库仑力,则结合反应的范特霍夫焓可能接近于零甚至为负,包括相对较强结合的情况。这些结果具有相当的普遍性,因此对于酶反应、合理药物设计、小分子与蛋白质的结合、蛋白质-蛋白质相互作用和蛋白质折叠等研究具有重要意义。