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Transport of Hop Bitter Acids across Intestinal Caco-2 Cell Monolayers

机译:啤酒花苦味酸跨肠Caco-2细胞单层的转运

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Several health-beneficial properties of hop bitter acids have been reported (inhibition of bone resorption and anticarcinogenic and anti-inflammatory activities); however, scientific data on the bioavailability of these compounds are lacking. As a first approach to study the bioavailability, the epithelial transport of hop α- and β-acids across Caco-2 monolayers was investigated, Hop acids were added either to the apical or to the basolateral chamber and, at various time points, amounts transported to the receiving compartment were determined. The monolayer integrity control was performed by using marker compounds (atenolol and propranolol), transepithelial electrical resistance (TEER) measurement, and determination of the fluorescein efflux. The TEER and fluorescein efflux confirmed the preservation of the monolayer integrity. The membrane permeability of the a-acids (apparent permeability coefficients for apical to basolateral transport (P_(appAB)) ranged from 14 x 10~(-6) to 41 x 10~(-6) cm/s) was determined to be substantially higher than that of the β-acids (P_(appAB) values ranging from 0.9 x 10~(-6) to 2.1 x 10~(-6) cm/s). Notably, the β-acids exhibited significantly different bidirectional P_(app) values with efflux ratios around 10. The involvement of carrier-mediated transport for β-acids (active efflux pathway by P-gp, BCRP, and/or MRP-2 type efflux pumps) could be confirmed by transport experiments with specific inhibitors (verapamil and indomethacin). It appears that a-acids are efficiently absorbed, whereas the permeability of β-acids is low. Limiting factors in the absorption of β-acids could involve P-gp and MRP-2 type efflux transporters and phase II metabolism.
机译:啤酒花苦味酸具有多种有益健康的特性(抑制骨吸收以及抗癌和抗炎活性);但是,缺乏有关这些化合物生物利用度的科学数据。作为研究生物利用度的第一种方法,研究了啤酒花α-和β-酸跨Caco-2单层的上皮运输,将啤酒花酸添加到顶端或基底外侧腔,并在不同时间点运输了一定量确定到接收室。通过使用标记化合物(阿替洛尔和普萘洛尔),跨上皮电阻(TEER)测量和荧光素外排的测定来进行单层完整性控制。 TEER和荧光素外排证实了单层完整性的保留。确定a-酸的膜渗透率(顶至基底外侧运输的表观渗透系数(P_(appAB))在14 x 10〜(-6)至41 x 10〜(-6)cm / s范围内)大大高于β-酸(P_(appAB)值范围从0.9 x 10〜(-6)到2.1 x 10〜(-6)cm / s)。值得注意的是,β-酸表现出显着不同的双向P_(app)值,流出比约为10。β-酸的载体介导转运参与(P-gp,BCRP和/或MRP-2型的主动流出途径)外排泵)可以通过使用特定抑制剂(维拉帕米和消炎痛)的转运实验来确认。看来α-酸被有效吸收,而β-酸的渗透性低。 β-酸吸收的限制因素可能涉及P-gp和MRP-2型外排转运蛋白以及II期代谢。

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