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使用Caco-2细胞单层模型对卡瓦内酯进行渗透性研究。

Permeability studies of Kavalactones using a Caco-2 cell monolayer model.

作者信息

Matthias A, Blanchfield J T, Penman K G, Bone K M, Toth I, Lehmann R P

机构信息

MediHerb Research Laboratories, Brisbane, Queensland, Australia.

出版信息

J Clin Pharm Ther. 2007 Jun;32(3):233-9. doi: 10.1111/j.1365-2710.2007.00810.x.

Abstract

OBJECTIVE

To examine the bioavailability of kavalactones in vitro and the possible differences in their bioavailability because of variations in either chemical structure or the method of extraction used.

RESEARCH DESIGN AND METHODS

Caco-2 cell monolayers were used to determine the potential bioavailability of kavalactones. Kavalactones were added to the apical layer and basolateral samples were taken over 150 min to examine the concentration diffusing across the cell monolayer. Kavalactone concentrations in these samples were determined by high pressure liquid chromatography.

RESULTS

Kavalactones were found to be potentially bioavailable as they all readily crossed the Caco-2 monolayers with apparent permeabilities (P(app)) increasing from 42 x 10(-6) cm/s and most exhibiting more than 70% crossing within 90 min. Not all differences in their bioavailability can be related to kavalactone structural differences as it appears that bioavailability may also be affected by co-extracted compounds. For example, the P(app) for kawain from ethanol extracts was higher than the values obtained for the same compound from water extracts or for the kavalactone alone.

CONCLUSIONS

While the extraction method used (ethanol or water) influences the total (but not the relative) concentrations of kavalactones, it does not markedly affect their bioavailability. Hence, any differences between an ethanolic or an aqueous extract in terms of the propensity of kava to cause liver damage is not because of differing kavalactone bioavailabilities.

摘要

目的

研究卡瓦内酯的体外生物利用度,以及由于化学结构或提取方法的差异可能导致的生物利用度差异。

研究设计与方法

采用Caco-2细胞单层模型来测定卡瓦内酯的潜在生物利用度。将卡瓦内酯添加到顶端层,并在150分钟内采集基底外侧样品,以检测穿过细胞单层的浓度。通过高压液相色谱法测定这些样品中的卡瓦内酯浓度。

结果

发现卡瓦内酯具有潜在的生物利用度,因为它们都能轻易穿过Caco-2细胞单层,表观渗透率(P(app))从42×10⁻⁶ cm/s增加,且大多数在90分钟内有超过70%的穿过率。并非所有生物利用度的差异都与卡瓦内酯的结构差异有关,因为生物利用度似乎也可能受到共提取物的影响。例如,乙醇提取物中卡哇因的P(app)高于水提取物中相同化合物或单独卡瓦内酯的P(app)值。

结论

虽然所使用的提取方法(乙醇或水)会影响卡瓦内酯的总浓度(但不影响相对浓度),但不会显著影响其生物利用度。因此,卡瓦乙醇提取物或水提取物在导致肝损伤倾向方面的任何差异并非由于卡瓦内酯生物利用度不同。

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