Zheng Liang, Zhu Lijun, Zhao Min, Shi Jian, Li Yuhuan, Yu Jia, Jiang Huangyu, Wu Jinjun, Tong Yunli, Liu Yuting, Hu Ming, Lu Linlin, Liu Zhongqiu
Department of Pharmaceutics, School of Pharmaceutical Sciences, Southern Medical University, Guangzhou, Guangdong, 510515, People's Republic of China.
International Institute for Translational Chinese Medicine, Guangzhou University of Chinese Medicine, Guangzhou, Guangdong, 510006, People's Republic of China.
AAPS J. 2016 Sep;18(5):1289-1299. doi: 10.1208/s12248-016-9951-9. Epub 2016 Jul 8.
Kaempferol is a well-known flavonoid; however, it lacks extensive pharmacokinetic studies. Phase II metabolic enzymes and efflux transporters play an important role in the disposition of flavonoids. This study aimed to investigate the mechanism by which phase II metabolic enzymes and efflux transporters determine the in vivo exposure of kaempferol. Pharmacokinetic analysis in Sprague-Dawley rats revealed that kaempferol was mostly biotransformed to conjugates, namely, kaempferol-3-glucuronide (K-3-G), kaempferol-7-glucuronide (K-7-G), and kaempferol-7-sulfate, in plasma. K-3-G represented the major metabolite. Compared with that in wild-type mice, pharmacokinetics in knockout FVB mice demonstrated that the absence of multidrug resistance protein 2 (MRP2) and breast cancer resistance protein (BCRP) significantly increased the area under the curve (AUC) of the conjugates. The lack of MRP1 resulted in a much lower AUC of the conjugates. Intestinal perfusion in rats revealed that the glucuronide conjugates were mainly excreted in the small intestine, but 7-sulfate was mainly excreted in the colon. In Caco-2 monolayers, K-7-G efflux toward the apical (AP) side was significantly higher than K-3-G efflux. In contrast, K-3-G efflux toward the basolateral (BL) side was significantly higher than K-7-G efflux. The BL-to-AP efflux was significantly reduced in the presence of the MRP2 inhibitor LTC4. The AP-to-BL efflux was significantly decreased in the presence of the BL-side MRPs inhibitor MK571. The BCRP inhibitor Ko143 decreased the glucuronide conjugate efflux. Therefore, kaempferol is mainly exposed as K-3-G in vivo, which is driven by phase II metabolic enzymes and efflux transporters (i.e., BCRP and MRPs).
山奈酚是一种著名的黄酮类化合物;然而,它缺乏广泛的药代动力学研究。II期代谢酶和外排转运体在黄酮类化合物的处置中起重要作用。本研究旨在探讨II期代谢酶和外排转运体决定山奈酚体内暴露量的机制。对Sprague-Dawley大鼠的药代动力学分析表明,山奈酚在血浆中大多被生物转化为结合物,即山奈酚-3-葡萄糖醛酸苷(K-3-G)、山奈酚-7-葡萄糖醛酸苷(K-7-G)和山奈酚-7-硫酸盐。K-3-G是主要代谢产物。与野生型小鼠相比,基因敲除FVB小鼠的药代动力学表明,多药耐药蛋白2(MRP2)和乳腺癌耐药蛋白(BCRP)的缺失显著增加了结合物的曲线下面积(AUC)。MRP1的缺失导致结合物的AUC低得多。大鼠的肠道灌注显示,葡萄糖醛酸结合物主要在小肠排泄,但7-硫酸盐主要在结肠排泄。在Caco-2单层细胞中,K-7-G向顶侧(AP)的外排显著高于K-3-G的外排。相反,K-3-G向基底外侧(BL)的外排显著高于K-7-G的外排。在存在MRP2抑制剂LTC4的情况下,BL到AP的外排显著降低。在存在BL侧MRPs抑制剂MK571的情况下,AP到BL的外排显著降低。BCRP抑制剂Ko143降低了葡萄糖醛酸结合物的外排。因此,山奈酚在体内主要以K-3-G的形式存在,这是由II期代谢酶和外排转运体(即BCRP和MRPs)驱动的。