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Investigation of the Factors Responsible for the Poor Oral Bioavailability of Acacetin in Rats: Physicochemical and Biopharmaceutical Aspects

Authors
Han, Dong-GyunCha, EunjuJoo, JeongminHwang, Ji SunKim, SanghyunPark, TaeukJeong, Yoo-SeongMaeng, Han-JooKim, Sang-BumYoon, In-Soo
Issue Date
Feb-2021
Publisher
MDPI
Keywords
Acacetin; Bioavailabil-ity; Gastrointestinal absorption; Solubility; Stability; Tissue metabolism
Citation
Pharmaceutics, v.13, no.2
Journal Title
Pharmaceutics
Volume
13
Number
2
URI
https://scholarworks.bwise.kr/gachon/handle/2020.sw.gachon/80511
DOI
10.3390/pharmaceutics13020175
ISSN
1999-4923
Abstract
Acacetin, an important ingredient of acacia honey and a component of several medicinal plants, exhibits therapeutic effects such as antioxidative, anticancer, anti-inflammatory, and anti-plasmodial activities. However, to date, studies reporting a systematic investigation of the in vivo fate of orally administered acacetin are limited. Moreover, the in vitro physicochemical and biopharmaceutical properties of acacetin in the gastrointestinal (GI) tract and their pharmacokinetic impacts remain unclear. Therefore, in this study, we aimed to systematically investigate the oral absorption and disposition of acacetin using relevant rat models. Acacetin exhibited poor solubility (≤119 ng/mL) and relatively low stability (27.5–62.0% remaining after 24 h) in pH 7 phosphate buffer and simulated GI fluids. A major portion (97.1%) of the initially injected acacetin dose re-mained unabsorbed in the jejunal segments, and the oral bioavailability of acacetin was very low at 2.34%. The systemic metabolism of acacetin occurred ubiquitously in various tissues (particularly in the liver, where it occurred most extensively), resulting in very high total plasma clearance of 199 ± 36 mL/min/kg. Collectively, the poor oral bioavailability of acacetin could be attributed mainly to its poor solubility and low GI luminal stability. © 2021 by the authors. Licensee MDPI, Basel, Switzerland.
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