RESUMO
We outline comparably simple molecular simulation techniques to elucidate the interactions that determine the polymorphism of carbamazepine. Starting from the established GAFF molecular mechanics model, only a small series of tailor-made improvements is needed to tackle the subtle differences in the interaction energies of polymorphs I - IV. On this basis, molecular dynamics simulations provide melting enthalpies at < 1 kcal/mol accuracy (0.2 kcal/mol for forms I-III) as compared to the experiment. Yet, the predicted stability ranking of III > I > II > IV only partially reproduces the experimentally observed III > I > IV > II series. Despite this limitation, we demonstrate how insights from molecular simulation offer the elucidation of possible factors for polymorph control. Apart from characterizing bulk crystals, we outline the evaluation of size-dependent profiles of crystallite formation energy. Contrasting the contributions of bulk, surface and edge terms to the formation energy of nano-scale precipitates, we suggest a multi-step nucleation mechanism leading from amorphous aggregates to crystallites. We argue that carbamazepine aggregates of less than â¼100 molecules adopt a spherical shape to minimize edge/surface energy - overcompensating the loss in bulk energy inherent to non-crystalline ordering in the inner core. In turn, for large crystallites polymorph form III is preferred, whilst suitable spatial confinement to crystallites of 100-500 carbamazepine molecules appears to promote form II.
