What question did this study set out to answer?

This study aims to evaluate how cocrystals of ketoconazole with acidic coformers can mitigate reduced absorption due to elevated gastric pH.

May 11, 2026Open Access

Cocrystal mitigates the effects of elevated gastric pH on oral absorption of weakly basic drugs: a case study with ketoconazole-succinic acid cocrystal on beagle dogs

Key Points

This study aims to evaluate how cocrystals of ketoconazole with acidic coformers can mitigate reduced absorption due to elevated gastric pH.
Conducted in vitro dissolution studies using cocrystals with fumaric, adipic, and succinic acids.
Performed bioavailability evaluations in beagle dogs under normal and elevated gastric pH conditions.
Measured drug absorption metrics such as AUC and C max after oral administration.
Cocrystal performance showed a reduction in AUC sensitivity by 1.3-fold compared to ketoconazole.
Cmax improved by 1.4-fold with the cocrystal versus a 7.5-fold reduction with ketoconazole at elevated pH.
In vitro studies indicated that ketoconazole alone exhibited a 12.3-fold reduction in AUC due to pH sensitivity.

Abstract

• Cocrystal dissolution pH-shift studies in vitro are good predictors of the superior bioavailability of cocrystal with a dibasic drug and diacidic coformers. • Cocrystals of weakly basic drugs with acidic coformers mitigate the negative effects of elevated gastric pH on drug absorption. • Cocrystals sustain drug supersaturation in vitro and improved in vivo absorption in beagle dogs. • The cocrystal approach reduces pH effects on dissolution and absorption. It is well documented that weakly basic drugs, such as ketoconazole (KTZ), will exhibit reduced oral absorption and lower bioavailability in elevated gastric pH conditions. Because this occurs frequently in patients taking medicines to reduce stomach acid, it is crucial to identify formulation strategies that ensure adequate drug exposure. The purpose of this work was to evaluate the in vitro and in vivo effects of KTZ cocrystals with acidic coformers in mitigating the negative effects of elevated gastric pH on KTZ dissolution and absorption after oral administration. Dissolution-supersaturation-precipitation in vitro studies were performed with drug and three KTZ cocrystals with fumaric (FUM), adipic (ADP), and succinic (SUC) acids, under a two-stage pH-shift micro dissolution method, to mimic the transfer from gastric to intestinal compartment. All cocrystals exhibited less sensitivity to elevated gastric pH than the drug. In vitro , cocrystals reduced the area under the curve (AUC) 2.6-fold compared to drug where AUC decreased 6.7-fold. Based on the superior performance observed during in vitro studies, the KTZ-SUC cocrystal was selected for bioavailability evaluation in beagle dogs treated with pentagastrin and famotidine to simulate normal and elevated gastric conditions. The cocrystal mitigated the negative effects of elevated dog gastric pH on KTZ absorption. It reduced the pH sensitivity of AUC (1.3 times) and C max (1.4 times). The drug exhibited high pH sensitivity with reduced AUC (12.3 times) and C max (7.5 times). These findings demonstrate that cocrystals of weakly basic BCS-class II drugs with acidic coformers promise to improve therapeutic outcomes that are otherwise limited by disease states or co-administration of drugs and food that increase gastric pH.

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Tucci et al. (Fri,) studied this question.

synapsesocial.com/papers/6a0171983a9f334c28271bbf https://doi.org/https://doi.org/10.1016/j.ejps.2026.107550

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