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Cocrystal Formation via Resorcinol-Urea Interactions: Naringenin and Carbamazepine

Authors
Lee, CheongCheonCho, A. YoungYoon, WoojinYun, HoseopKang, Jeong WonLee, Jonghwi
Issue Date
Jul-2019
Publisher
AMER CHEMICAL SOC
Citation
CRYSTAL GROWTH & DESIGN, v.19, no.7, pp 3807 - 3814
Pages
8
Journal Title
CRYSTAL GROWTH & DESIGN
Volume
19
Number
7
Start Page
3807
End Page
3814
URI
https://scholarworks.bwise.kr/cau/handle/2019.sw.cau/32856
DOI
10.1021/acs.cgd.9b00269
ISSN
1528-7483
1528-7505
Abstract
Improving the stability, bioavailability, and processability of active pharmaceutical ingredients (APIs) has been the key research goal in the field of pharmaceutical crystallization. Cocrystallization has been considered as an effective route to achieve this goal, and intense research over decades has revealed cocrystals of many APIs. However, most cocrystal formers have been designed based primarily on their molecular interactions not their health benefits. Herein, we choose naringenin (N), a natural flavonoid, as a novel cocrystal former as it has many health efficacies and the ability to form specific interactions. At a 1:1 stoichiometric ratio, N successfully forms a cocrystal with carbamazepine (CBZ), whose plasma concentration is known to be improved by natural flavonoids such as N. The resorcinol functional group of N and the urea functional group of CBZ are connected through hydrogen bonds, and the improved stability of the cocrystal seems to originate from this structure. The melting temperature of the cocrystal is 262 degrees C, which is higher than those of CBZ and N, and the better stability of the cocrystal is further confirmed by the observation of enhanced hydration stability (up to 30 days at 93% RH). This novel strategy of cocrystallization using natural flavonoids could improve the commercialization potential of API cocrystals.
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공과대학 (화학공학과)
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