Compromised in vitro dissolution and membrane transport of multidrug amorphous formulations

Amjad Alhalaweh; Christel A S Bergström; Lynne S Taylor

doi:10.1016/j.jconrel.2016.03.028

Compromised in vitro dissolution and membrane transport of multidrug amorphous formulations

J Control Release. 2016 May 10:229:172-182. doi: 10.1016/j.jconrel.2016.03.028. Epub 2016 Mar 19.

Authors

Amjad Alhalaweh¹, Christel A S Bergström², Lynne S Taylor³

Affiliations

¹ Department of Industrial and Physical Pharmacy, College of Pharmacy, Purdue University, West Lafayette, IN, 47907, United States.
² Department of Pharmacy, Uppsala University, Uppsala Biomedical Centre, P.O. Box 580, SE-751 23 Uppsala, Sweden.
³ Department of Industrial and Physical Pharmacy, College of Pharmacy, Purdue University, West Lafayette, IN, 47907, United States. Electronic address: lstaylor@purdue.edu.

PMID: 27006280
DOI: 10.1016/j.jconrel.2016.03.028

Abstract

Herein, the thermodynamic properties of solutions evolving from the non-sink dissolution of amorphous solid dispersions (ASDs) containing two or more drugs have been evaluated, focusing on the maximum achievable supersaturation and tendency of the system to undergo liquid-liquid phase separation (LLPS). Ritonavir (RTV) and atazanavir (ATV) were co-formulated with polyvinylpyrrolidone to produce ASDs with different molar ratios of each drug, and the dissolution profile of each drug was studied under non-sink conditions. The phase behavior of the supersaturated solutions generated by ASD dissolution was compared to that of supersaturated solutions generated by antisolvent addition. Dissolution of an ASD containing RTV, ATV and lopinavir (LPV) was also investigated. A thermodynamic model was used to predict the maximum achievable supersaturation for ASDs containing two and three drugs. In addition, a transport study with Caco-2 cells was conducted to evaluate the impact of co-addition of drugs on membrane transport. It was found that the formulation containing a 1:1 molar ratio of RTV and ATV achieved only 50% of the supersaturation attained by dissolution of the single drug systems. The maximum achievable concentration of ATV decreased linearly as the mole fraction of ATV in the formulation decreased and a similar trend was observed for RTV. For the dispersion containing a 1:1:1 molar ratio of RTV, ATV and LPV, the maximum concentration of each drug was only one third of that achieved for the single drug formulations. The decrease in the achievable supersaturation was well-predicted by the thermodynamic model for both the binary and ternary drug combinations. These observations can be explained by a decrease in the concentration at which the drugs undergo LLPS in the presence of other miscible drugs, thereby reducing the maximum achievable supersaturation of each drug. The reduced free drug concentration was reflected by a decreased flux across Caco-2 cells for the drug combinations compared to drug alone. This study sheds light on the complex dissolution and solution phase behavior of multicomponent amorphous dosage forms, in particular those containing poorly water soluble drugs, which may undergo supersaturation in vivo.

Keywords: Amorphous; Coamorphous; Dissolution; Multicomponent; Solubility; Supersaturation.

Publication types

Research Support, U.S. Gov't, Non-P.H.S.

MeSH terms

Atazanavir Sulfate* / chemistry
Atazanavir Sulfate* / pharmacology
Biological Transport
Caco-2 Cells
Cell Membrane / metabolism
Dosage Forms
Drug Compounding
Drug Liberation
HIV Protease Inhibitors* / chemistry
HIV Protease Inhibitors* / pharmacology
Humans
Lopinavir* / chemistry
Lopinavir* / pharmacology
Ritonavir* / chemistry
Ritonavir* / pharmacology
Solubility

Substances

Dosage Forms
HIV Protease Inhibitors
Lopinavir
Atazanavir Sulfate
Ritonavir