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Crystallisation and physicochemical property characterisation of conformationally-locked co-crystals of fenamic acid derivatives

By Wittering, KE; Agnew, LRKlapwijk, AR; Robertson, K; Cousen, AJP; Cruickshank, DL; Wilson, CC

Published on

Abstract

Polymorphism in drug compounds can cause significant problems for industrial-scale production and so a method for restricting the conformational freedom of the target compound whilst retaining desired chemical properties is highly beneficial to the pharmaceutical industry. Co-crystallisation is commonly used to alter the structure of an active pharmaceutical ingredient (API) without affecting its activity. A comprehensive co-crystal screen of four fenamic acid derivatives affords a strictly limited number of co-crystals. These show no evidence of polymorphism, although some of the parent APIs exhibit significant polymorphism. Two of these co-crystals, of mefenamic acid and tolfenamic acid with 4,4'-bipyridine, were previously unknown and are studied using X-ray diffraction. Co-crystals from this screen are fully characterised and display comparable solubility and stability with respect to the parent APIs; no phase transformations have been identified. A range of crystallisation techniques, including cooling and grinding methods, are shown to afford single polymorphic forms for each of the co-crystals.

Journal

Crystal Engineering Communications. Volume 17, 2015, 3610-3618

DOI

10.1039/c5ce00297d

Type of publication

Peer-reviewed journal

Affiliations

  • University of Bath

Article Classification

Research Article

Classification Areas

  • API

Tags