Understanding the Effects of a Polymer on the Surface Dissolution of Pharmaceutical Cocrystals Using Combined Experimental and Molecular Dynamics Simulation Approaches

Preyanthiny Kirubakaran; Ke Wang; Ian Rosbottom; Richard Barrie Michael Cross; Mingzhong Li

doi:10.1021/acs.molpharmaceut.9b00955

Understanding the Effects of a Polymer on the Surface Dissolution of Pharmaceutical Cocrystals Using Combined Experimental and Molecular Dynamics Simulation Approaches

Mol Pharm. 2020 Feb 3;17(2):517-529. doi: 10.1021/acs.molpharmaceut.9b00955. Epub 2020 Jan 7.

Authors

Preyanthiny Kirubakaran¹, Ke Wang¹, Ian Rosbottom², Richard Barrie Michael Cross³, Mingzhong Li¹

Affiliations

¹ School of Pharmacy , De Montfort University , The Gateway , Leicester LE1 9BH , U.K.
² Department of Chemical Engineering , Imperial College London , London SW7 2BX , U.K.
³ School of Engineering , De Montfort University , The Gateway , Leicester LE1 9BH , U.K.

PMID: 31887053
DOI: 10.1021/acs.molpharmaceut.9b00955

Abstract

The molecular interactions between the surfaces of cocrystals [i.e., flufenamic acid and theophylline (FFA-TP), flufenamic acid and nicotinamide (FFA-NIC), and carbamazepine and nicotinamide (CBZ-NIC)] and the polymers [i.e., polyethylene glycol (PEG), polyvinylpyrrolidone (PVP), and copolymer of vinylpyrrolidone (60%)/vinyl acetate (40%) (PVP-VA)] were investigated through combined experimental and molecular dynamics simulation approaches to resolve the mechanisms of cocrystal dissolution and precipitation. It was found that adsorption of the polymers on the surfaces of cocrystals might prevent the precipitation of the parent drug and alter the dissolution rate. The effect of polymers on precipitation could be determined by the cocrystal dissolution rate, the interactions of polymers with the surfaces of cocrystals, the characters of the noncovalent bonds formed between the polymers and the cocrystal surfaces, and the mobility and conformation of the polymers. The etching experiments of single cocrystals revealed that FFA-NIC and CBZ-NIC appeared as surface precipitation cocrystals while FFA-TP could lead to bulk precipitation. Both PVP and PVP-VA were good precipitation inhibitors for FFA-NIC, and they could completely inhibit the recrystallization of FFA III on the surfaces of dissolving cocrystals. In addition, as the adsorption of the polymer was slower than dissolution rate of the cocrystals, PVP and PVP-VA could only partially inhibit the recrystallization of CBZ dihydrate on the surface of CBZ-NIC. While PEG had no inhibitory effect on the surface crystallization of FFA-NIC and CBZ-NIC, due to its weak interactions with the surfaces of the cocrystals, it enhanced the dissolution performance of FFA-TP. In contrast, PVP and PVP-VA reduced the dissolution rate of FFA-TP and subsequently undermined the performance of cocrystals. Taken together, the approach of combining experimental and molecular dynamics simulation provided insights into the mechanisms of cocrystal dissolution as well as the polymers acting as inhibitory excipients for precipitation/recrystallization, making contribution to the development of novel formulations.

Keywords: carbamazepine cocrystals; cocrystals; flufenamic acid cocrystals; molecular dynamics; molecular modeling; polymer; precipitation and dissolution inhibitor.

MeSH terms

Adsorption
Carbamazepine / chemistry*
Chemical Precipitation
Crystallization
Drug Compounding / methods
Drug Liberation
Excipients / chemistry
Flufenamic Acid / chemistry*
Molecular Dynamics Simulation
Niacinamide / chemistry*
Polyethylene Glycols / chemistry*
Povidone / chemistry*
Pyrrolidines / chemistry*
Solubility
Theophylline / chemistry*
Vinyl Compounds / chemistry*

Substances

Excipients
Pyrrolidines
Vinyl Compounds
poly(vinylpyrrolidone-co-vinyl-acetate)
Niacinamide
Carbamazepine
Polyethylene Glycols
Flufenamic Acid
Theophylline
Povidone