Role of Molecular, Crystal, and Surface Chemistry in Directing the Crystallization of Entacapone Polymorphs on the Au(111) Template Surface

Abstract: The pharmaceutical compound entacapone ((E)-2-cyano-3-(3,4-dihydroxy-5-nitrophenyl)-N,N-diethylprop-2-enamide) is important in the treatment of Parkinson’s disease, exhibiting interesting polymorphic behavior upon crystallization from solution. It consistently produces its stable form A with a uniform crystal size distribution on the surface of an Au(111) template while concomitantly forming its metastable form D within the same bulk solution. Molecular modeling using empirical atomistic force-fields reveals m… Show more

“…In this, at the nucleation on-set point, the higher supersaturations would produce smaller critical cluster sizes, stabilizing the metastable form. 50 , 72 , 99 The PXRD analysis is supported by reference DSC data for forms I and II of ritonavir which are given in Figure S1 ( Supporting Information ) and reveal endothermic melting peaks at around 123 °C for form I and 126 °C for form II. 84 , 100 The observed melting points for the form I isolated from the four solvents were found to fluctuate slightly from 123 °C in toluene to 125 °C in acetone with their enthalpies of fusion calculated based on the DSC data increasing from 38.43 to 41.19 kJ mol –1 and the full widths at half-maximum decreasing from 3.45 to 2.21 °C [see Table S1 ( Supporting Information ) for further details], reflecting, perhaps, the different crystallinity and morphology of the associated solid forms.…”

“…In this, at the nucleation on-set point, the higher supersaturations would produce smaller critical cluster sizes, stabilizing the metastable form. 50,72,99 The PXRD analysis is supported by reference DSC S1 (Supporting Information) for further details], reflecting, perhaps, the different crystallinity and morphology of the associated solid forms.…”

“…In silico methods, such as molecular dynamics (MD) simulations, have been widely used to capture the dynamical behavior of the explicit intermolecular interactions within the solution phase both qualitatively and also quantitatively by developing an understanding of the molecular and intermolecular assembly behavior during the crystal nucleation process associated with crystallization from solutions (e.g., refs ,– ). Recently, some detailed methods have been developed to characterize the propensity of incipient bulk synthons within the solution state through the targeted analysis of the MD trajectory files. ,, …”

Influence of Solvent Selection on the Crystallizability and Polymorphic Selectivity Associated with the Formation of the “Disappeared” Form I Polymorph of Ritonavir

“…In this, at the nucleation on-set point, the higher supersaturations would produce smaller critical cluster sizes, stabilizing the metastable form. 50 , 72 , 99 The PXRD analysis is supported by reference DSC data for forms I and II of ritonavir which are given in Figure S1 ( Supporting Information ) and reveal endothermic melting peaks at around 123 °C for form I and 126 °C for form II. 84 , 100 The observed melting points for the form I isolated from the four solvents were found to fluctuate slightly from 123 °C in toluene to 125 °C in acetone with their enthalpies of fusion calculated based on the DSC data increasing from 38.43 to 41.19 kJ mol –1 and the full widths at half-maximum decreasing from 3.45 to 2.21 °C [see Table S1 ( Supporting Information ) for further details], reflecting, perhaps, the different crystallinity and morphology of the associated solid forms.…”

“…In this, at the nucleation on-set point, the higher supersaturations would produce smaller critical cluster sizes, stabilizing the metastable form. 50,72,99 The PXRD analysis is supported by reference DSC S1 (Supporting Information) for further details], reflecting, perhaps, the different crystallinity and morphology of the associated solid forms.…”

“…In silico methods, such as molecular dynamics (MD) simulations, have been widely used to capture the dynamical behavior of the explicit intermolecular interactions within the solution phase both qualitatively and also quantitatively by developing an understanding of the molecular and intermolecular assembly behavior during the crystal nucleation process associated with crystallization from solutions (e.g., refs ,– ). Recently, some detailed methods have been developed to characterize the propensity of incipient bulk synthons within the solution state through the targeted analysis of the MD trajectory files. ,, …”

Influence of Solvent Selection on the Crystallizability and Polymorphic Selectivity Associated with the Formation of the “Disappeared” Form I Polymorph of Ritonavir

“…The development of computational molecular-scale modelling has contributed significantly to the understanding of the thermodynamic properties within the solution state, especially when integrated with experimental data. A variety of molecular-scale computation methods have been successfully applied to the characterisation of the solid state and solution chemistry, 2,5,16,24–41 such as ab initio quantum mechanics using density functional theory (DFT) and molecular dynamics (MD) and molecular mechanics (MM) simulations using parametrised empirical interatomic force fields. Although providing high accuracy, DFT calculations and MD simulations can make a significantly high demand on both computer power and calculation time.…”

Influence of the crystallisation solution environment on the structural pathway from solute solvation to the polymorphic forms of tolfenamic acid

Calculating the surface energies of crystals on a face-specific and whole particle basis: Case study of the α- and β-polymorphic forms of L-glutamic acid