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Colon-Targeted Trans-Cinnamic Acid Ameliorates Rat Colitis by Activating GPR109A

Changyu Kang, Jaejeong Kim, Sanghyun Ju, Heeyeong Cho, Ho Kim, In‐Soo Yoon, Jin‐Wook Yoo, Yunjin Jung

2022Pharmaceutics16 citationsDOIOpen Access PDF

Abstract

We designed colon-targeted trans-cinnamic acid (tCA) and synthesized its conjugates with glutamic acid (tCA-GA) and aspartic acid (tCA-AA). We evaluated the anti-colitic activity of colon-targeted tCA using a dinitrobenzenesulfonic acid-induced rat colitis model. The conjugates lowered the distribution coefficient and Caco-2 cell permeability of tCA and converted to tCA in the cecum, with higher rates and percentages with tCA-GA than with tCA-AA. Following oral gavage, tCA-GA delivered a higher amount of tCA to the cecum and exhibited better anti-colitic effects than tCA and sulfasalazine (SSZ), which is the current treatment for inflammatory bowel disease. In the cellular assay, tCA acted as a full agonist of GPR109A (EC50: 530 µM). The anti-colitic effects of tCA-GA were significantly compromised by the co-administration of the GPR109A antagonist, mepenzolate. Collectively, colon-targeted tCA potentiated the anti-colitic activity of tCA by effectively activating GPR109A in the inflamed colon, enabling tCA to elicit therapeutic superiority over SSZ.

Topics & Concepts

ColitisPharmacologyChemistryCecumTricarboxylic acidBiochemistryMedicineInternal medicineMetabolismCitric acid cycleInflammatory Bowel DiseaseDrug Transport and Resistance MechanismsHelicobacter pylori-related gastroenterology studies