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Kaempferol suppression of acute colitis is regulated by the efflux transporters BCRP and MRP2

山奈酚 多药耐药蛋白2 化学 药理学 流出 Abcg2型 生物利用度 CYP3A4型 药代动力学 运输机 生物化学 类黄酮 ATP结合盒运输机 生物 新陈代谢 细胞色素P450 基因 抗氧化剂
作者
Yuanyuan Liu,Yiyan Lu,Xiaoyan Li,Zerong Zhang,Lizhu Sun,Ying Wang,Zhuoru He,Zhongqiu Liu,Lijun Zhu,Ling Fu
出处
期刊:European Journal of Pharmaceutical Sciences [Elsevier]
卷期号:179: 106303-106303 被引量:7
标识
DOI:10.1016/j.ejps.2022.106303
摘要

The bioavailability of most flavonoids is low but effective in vivo; however, the mechanism of the efficacy of flavonoids has not been elucidated. Kaempferol is typical flavonoids., preliminary research indicates that kaempferol has a significant anti-colon cancer and anti-inflammatory effect. We reported previously that the triple recycling pathways significantly increase the local bioavailability of flavonoids and prolong the residence time of flavonoids in the liver and intestines, which is likely the mode by which flavonoids exert local efficacy. Notably, Efflux transporters (ETs), such as Breast cancer resistance protein (BCRP) and Multi drug resistance-associated protein 2 (MRP2), are the main regulatory molecules of the enterohepatic triple recycling pathways. Thus, our current study explored the regulation of kaempferol by BCRP and MRP2 and the role of BCRP and MRP2 in the suppression of Dextran sulfate sodium (DSS)-induced colitis by kaempferol. Herein, four mouse model was constructed, and the Ultra-high-performance liquid chromatography-tandem mass spectrometry (UHPLC–MS/MS) method was established to simultaneously quantify kaempferol and its 3 metabolites and investigate the oral pharmacokinetic characteristics and tissue distribution of these compounds. In Bcrp−/−-Mrp2−/− mice, the movement of kaempferol via the enterohepatic triple recycling was blocked, and the preventative and therapeutic effects of this compound on acute colitis were inhibited. BCRP and MRP2 defects hindered the efflux of kaempferol and its phase II metabolites and increased the plasma levels. Our study revealed that the disposal of kaempferol was regulated by the ETs BCRP and MRP2, and most importantly, the results will help elucidate the mechanism by which kaempferol suppresses the transformation of colitis into colon cancer.
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