TY - DATA T1 - Differential Binding Models for Isothermal Titration Calorimetry: Moving beyond the Wiseman Isotherm PY - 2013/07/25 AU - Isaac Herrera AU - Mitchell A. Winnik UR - https://acs.figshare.com/articles/journal_contribution/Differential_Binding_Models_for_Isothermal_Titration_Calorimetry_Moving_beyond_the_Wiseman_Isotherm/2392948 DO - 10.1021/jp311812a.s001 L4 - https://ndownloader.figshare.com/files/4032640 KW - dimensionless parameter c KW - study ITC experiments KW - receptor KW - Differential Binding Models KW - binding sites KW - Isothermal Titration Calorimetry KW - sequential binding model KW - binding polynomial formalism KW - binding interaction KW - DBM KW - MT N2 - We present a set of model-independent differential equations to analyze isothermal titration calorimetry (ITC) experiments. In contrast with previous approaches that begin with specific assumptions about the number of binding sites and the interactions among them (e.g., sequential, independent, cooperative), our derivation makes more general assumptions, such that a receptor with multiple sites for one type of ligand species (homotropic binding) can be studied with the same analytical expression. Our approach is based on the binding polynomial formalism, and the resulting analytical expressions can be extended to account for any number of binding sites and any type of binding interaction among them. We refer to the set of model-independent differential equations to study ITC experiments as a differential binding model (DBM). To demonstrate the flexibility of our DBM, we present the analytical expressions to study receptors with one or two binding sites. The DBM for a receptor with one site is equivalent to the Wiseman isotherm but with a more intuitive representation that depends on the binding polynomial and the dimensionless parameter c = K·MT, where K is the binding constant and MT the total receptor concentration. In addition, we show how to constrain the general DBM for a receptor with two sites to represent sequential, independent, or cooperative binding interactions between the sites. We use the sequential binding model to study the binding interaction between Gd­(III) and citrate anions. In addition, we simulate calorimetry titrations of receptors with positive, negative, and noncooperative interactions between the two binding sites. Finally, we derive a DBM for titrations of receptors with n-independent binding sites. ER -