PT - JOURNAL ARTICLE AU - Jacob Peacock AU - James B. Jaynes TI - Using competition assays to quantitatively model cooperative binding by transcription factors and other ligands AID - 10.1101/170340 DP - 2017 Jan 01 TA - bioRxiv PG - 170340 4099 - http://biorxiv.org/content/early/2017/07/31/170340.short 4100 - http://biorxiv.org/content/early/2017/07/31/170340.full AB - BACKGROUND The affinities of DNA binding proteins for target sites can be used to model the regulation of gene expression. These proteins can bind to DNA cooperatively, strongly impacting their affinity and specificity. However, current methods for measuring cooperativity do not provide the means to accurately predict binding behavior over a wide range of concentrations.METHODS We use standard computational and mathematical methods, and develop novel methods as described in Results.RESULTS We explore some complexities of cooperative binding, and develop an improved method for relating in vitro measurements to in vivo function, based on ternary complex formation. We derive expressions for the equilibria among the various complexes, and explore the limitations of binding experiments that model the system using a single parameter. We describe how to use single-ligand binding and ternary complex formation in tandem to determine parameters that have thermodynamic relevance. We develop an improved method for finding both single-ligand dissociation constants and concentrations simultaneously. We show how the cooperativity factor can be found when only one of the single-protein dissociation constants can be measured.CONCLUSIONS The methods that we develop constitute an optimized approach to accurately model cooperative binding.GENERAL SIGNIFICANCE The expressions and methods we develop for modeling and analyzing DNA binding and cooperativity are applicable to most cases where multiple ligands bind to distinct sites on a common substrate. The parameters determined using these methods can be fed into models of higher-order cooperativity to increase their predictive power.HIGHLIGHTSHill plots remain prominent in biology, but can mask cooperativityEffective modeling of binding by two ligands requires the use of 3 parametersWe develop novel ways to find these parameters for two cooperating ligandsWe show how they can be used to enhance the power of established methodsWe describe how this framework can be extended to multiple cooperating ligands