Abstract Drug discovery and development process is a long and expensive process. The average cost of a new drug from laboratory to market is about US$500 to US$880 million and it takes ten to fifteen years to complete all the process. Three important studies in this thesis were performed to improve the efficiency of the discovery and development process. Firstly, a useful engineering data bank of solubility, polymorphism, crystal habits and crystallinity by solvent screening for acetaminophen would be established and a robust, miniature solvent screening method would be introduced. Secondary, a new chip method for interfacial screening between acetaminophen and templates was developed. This method could be used to predict and avoid the problems caused by templates during manufacturing and was also in miniature scale experiments. Thirdly, a solid dispersion formulation screening of acetaminophen and sucrose were investigated. The dispersion sample showed a better dissolution behavior than pure acetaminophen and sweet taste of sucrose has a potential value of masking the bitterness of acetaminophen. Acetaminophen was chosen as the active pharmaceutical ingredient (API) because of its commercial value and rich literatures. But the investigating methods in this thesis, could also be applied to some other APIs or drug candidates or simple organic materials.