首页> 外文期刊>Journal of Agricultural and Food Chemistry >In Vitro Pharmacokinetic Characterization of Mulberroside A, the Main Polyhydroxylated Stilbene in Mulberry (Moms alba L), and Its Bacterial Metabolite Oxyresveratrol in Traditional Oral Use
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In Vitro Pharmacokinetic Characterization of Mulberroside A, the Main Polyhydroxylated Stilbene in Mulberry (Moms alba L), and Its Bacterial Metabolite Oxyresveratrol in Traditional Oral Use

机译:桑树糖苷A,桑树中的主要多羟基二苯乙烯类化合物(Moms alba L)的体外药代动力学表征及其传统口服方式中的细菌代谢产物氧白藜芦醇

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Mulberroside A (MulA) is one of the main bioactive constituents in mulberry (Moms alba L.). This study examined the determining factors for previously reported oral pharmacokinetic profiles of MulA and its bacterial metabolite oxyresveratrol (OXY) on in vitro models. When incubated anaerobically with intestinal bacteria, MulA underwent rapid deglycosylation and generated two monoglucosides and its aglycone OXY sequentially. MulA exhibited a poor permeability and predominantly traversed Caco-2 cells via passive diffusion; yet, the permeation of OXY across Caco-2 cells was much more rapid and involved efflux (both p-glycoprotein and MRPs)-mediated mechanisms. Moreover, OXY underwent extensive hepatic glucuronidation; yet, the parent MulA was kept intact in liver subcellular preparations. There was insignificant species difference in intestinal bacterial conversion of MulA and the extent of OXY hepatic glucuronidation between humans and rats, while OXY exhibited a distinct positional preference of glucuronidation in the two species. Overall, these findings revealed a key role of intestinal bacterial conversion in absorption and systemic exposure of MulA and its resultant bacterial metabolite OXY in oral route in humans and rats and warranted further investigational emphasis on OXY and its hepatic metabolites for understanding the benefits of mulberry.
机译:桑树甙A(MulA)是桑树(Moms alba L.)中的主要生物活性成分之一。这项研究检查了体外模型上先前报道的MulA及其细菌代谢产物氧白藜芦醇(OXY)的口服药代动力学特征的决定因素。当与肠道细菌厌氧孵育时,MulA会进行快速去糖基化,并依次生成两个单糖苷及其糖苷配基OXY。 MulA表现出差的渗透性并且主要通过被动扩散横穿了Caco-2细胞。然而,OXY跨Caco-2细胞的渗透要快得多,并且涉及外排(p-糖蛋白和MRPs)介导的机制。此外,OXY经历了广泛的肝葡萄糖醛酸化;然而,母体MulA在肝亚细胞制剂中保持完整。在人类和大鼠之间,MulA的肠道细菌转化和OXY肝葡萄糖醛酸化程度的种类差异不明显,而OXY在这两种物种中表现出明显的葡萄糖醛酸化位置偏好。总体而言,这些发现揭示了肠道细菌转化在人类和大鼠口服途径中对MulA及其所产生的细菌代谢产物OXY的吸收和全身暴露中的关键作用,并且有必要进一步研究OXY及其肝代谢产物以了解桑树的益处。

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