Issue 19, 2019

Simultaneously enhancing the in vitro/in vivo performances of acetazolamide using proline as a zwitterionic coformer for cocrystallization

Abstract

With the objective to improve the physicochemical properties and optimize pharmacokinetic performances of acetazolamide (ACA), a new zwitterionic cocrystal of ACA with proline (PRO), namely, ACA-PRO, was synthesized and characterized. The single-crystal X-ray diffraction analysis revealed that the cocrystal has a component ratio of 1 : 1 and is dominated by a three dimensional hydrogen bonding supramolecular structure. The water solubility and permeability of ACA in the cocrystal were simultaneously enhanced compared with pure ACA in physiological pH environments. The in vivo pharmacokinetic evaluation indicated that the relative bioavailability of ACA from the cocrystal was enhanced by 2.68-fold. The present investigation not only provides an alternative approach for optimizing physicochemical and pharmacokinetic properties of BCS class-IV drugs without changing the molecular structures and intrinsic bioactivities, but also enriches the current understanding of the structures of zwitterionic cocrystals and their behaviors in vitro and in vivo.

Graphical abstract: Simultaneously enhancing the in vitro/in vivo performances of acetazolamide using proline as a zwitterionic coformer for cocrystallization

Supplementary files

Article information

Article type
Paper
Submitted
26 Feb 2019
Accepted
15 Apr 2019
First published
17 Apr 2019

CrystEngComm, 2019,21, 3064-3073

Simultaneously enhancing the in vitro/in vivo performances of acetazolamide using proline as a zwitterionic coformer for cocrystallization

Y. Song, L. Wang, F. Liu, Y. Li, Z. Wu and C. Yan, CrystEngComm, 2019, 21, 3064 DOI: 10.1039/C9CE00270G

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