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西洋蒲公英和白花西洋蒲公英提取物刺激 Bauer 酰胺 8 和 10 及酮 24 的葡萄糖醛酸化和基底外侧转运,并抑制 Caco-2 细胞中的 P-糖蛋白转运体。

Echinacea sanguinea and Echinacea pallida extracts stimulate glucuronidation and basolateral transfer of Bauer alkamides 8 and 10 and ketone 24 and inhibit P-glycoprotein transporter in Caco-2 cells.

机构信息

Center for Research on Botanical Dietary Supplements, Iowa State University, Ames, IA 50011, USA.

出版信息

Planta Med. 2013 Mar;79(3-4):266-74. doi: 10.1055/s-0032-1328198. Epub 2013 Feb 13.

DOI:10.1055/s-0032-1328198
PMID:23408271
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3758111/
Abstract

The use of Echinacea as a medicinal herb is prominent in the United States, and many studies have assessed the effectiveness of Echinacea as an immunomodulator. We hypothesized that Bauer alkamides 8, 10, and 11 and ketone 24 were absorbed similarly either as pure compounds or from Echinacea sanguinea and Echinacea pallida ethanol extracts, and that these Echinacea extracts could inhibit the P-glycoprotein transporter in Caco-2 human intestinal epithelial cells. Using HPLC analysis, the permeation rate of Bauer alkamides by passive diffusion across Caco-2 cells corresponded with compound hydrophilicity (alkamide 8 > 10 > 11), independent of the plant extract matrix. Both Echinacea ethanol extracts stimulated apparent glucuronidation and basolateral efflux of glucuronides of alkamides 8 and 10 but not alkamide 11. Bauer ketone 24 was totally metabolized to more hydrophilic metabolites when administered as a single compound, but was also glucuronidated when present in Echinacea extracts. Bauer alkamides 8, 10, and 11 (175-230 µM) and ethanol extracts of E. sanguinea (1 mg/mL, containing ~ 90 µM total alkamides) and E. pallida (5 mg/mL, containing 285 µM total alkamides) decreased the efflux of the P-glycoprotein transporter probe calcein-AM from Caco-2 cells. These results suggest that other constituents in these Echinacea extracts facilitated the metabolism and efflux of alkamides and ketones, which might improve therapeutic benefits. Alkamides and Echinacea extracts might be useful in potentiating some chemotherapeutics, which are substrates for the P-glycoprotein transporter.

摘要

作为一种药用植物,紫锥菊在美国的应用非常突出,许多研究都评估了紫锥菊作为免疫调节剂的功效。我们假设 Bauer 酰胺 8、10 和 11 以及酮 24 作为纯化合物或从紫松果菊和白花紫锥菊乙醇提取物中被吸收的方式相似,并且这些紫锥菊提取物可以抑制 Caco-2 人肠上皮细胞中的 P-糖蛋白转运体。使用 HPLC 分析,Bauer 酰胺通过 Caco-2 细胞的被动扩散的渗透速率与化合物的亲水性相对应(酰胺 8 > 10 > 11),与植物提取物基质无关。两种紫锥菊乙醇提取物均刺激酰胺 8 和 10 的葡萄糖醛酸化和基底外侧流出,但不刺激酰胺 11。当作为单一化合物给药时,Bauer 酮 24 完全代谢为更亲水的代谢物,但在紫锥菊提取物中也被葡萄糖醛酸化。Bauer 酰胺 8、10 和 11(175-230 µM)和紫松果菊(1 mg/mL,含约 90 µM 总酰胺)和白花紫锥菊(5 mg/mL,含 285 µM 总酰胺)的乙醇提取物从 Caco-2 细胞中降低了 P-糖蛋白转运体探针 calcein-AM 的外排。这些结果表明,这些紫锥菊提取物中的其他成分促进了酰胺和酮的代谢和外排,这可能提高治疗效果。酰胺和紫锥菊提取物可能有助于增强某些化学治疗药物的疗效,这些药物是 P-糖蛋白转运体的底物。

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