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培养胃上皮细胞单层中的绿原酸吸收和代谢。

Absorption and metabolism of chlorogenic acids in cultured gastric epithelial monolayers.

机构信息

School of Food Science and Nutrition, University of Leeds, Leeds, UK.

出版信息

Drug Metab Dispos. 2011 Dec;39(12):2338-46. doi: 10.1124/dmd.111.040147. Epub 2011 Sep 21.

Abstract

Gastric absorption of feruloylquinic acid and di-O-caffeoylquinic acid analogs has never been investigated despite their potential contribution to the proposed beneficial health effects leading to reduced risk of type 2 diabetes. Using a cultured gastric epithelial model, with an acidic apical pH, the relative permeability coefficients (P(app)) and metabolic fate of a series of chlorogenic acids (CGAs) were investigated. Mechanistic studies were performed in the apical to basal direction and demonstrated differential rates of absorption for different CGA subgroups. For the first time, we show intact absorption of feruloylquinic acids and caffeoylquinic acid lactones across the gastric epithelium (P(app) ∼ 0.2 cm/s). Transport seemed to be mainly by passive diffusion, because good linearity was observed over the incubation period and test concentrations, and we speculate that a potential carrier-mediated component may be involved in uptake of certain 4-acyl CGA isomers. In contrast, absorption of intact di-O-caffeoylquinic acids was rapid (P(app) ∼ 2-10 cm/s) but nonlinear with respect to time and concentration dependence, which was potentially limited by interaction with an efflux transporter and/or pH gradient dependence. For the first time, methylation is shown in gastric mucosa. Furthermore, isoferulic acid, dimethoxycinnamic acid, and ferulic acid were identified as novel gastric metabolites of CGA biotransformation. We propose that the stomach is the first location for the release of hydroxycinnamic acids, which could explain their early detection after coffee consumption.

摘要

尽管对咖啡酰奎尼酸和二咖啡酰奎尼酸类似物具有降低 2 型糖尿病风险的潜在有益健康作用已有研究,但胃对它们的吸收情况尚未被研究过。本研究使用具有酸性顶端 pH 值的培养胃上皮模型,考察了一系列绿原酸(CGAs)的相对渗透系数(P(app))和代谢命运。在顶端到基底的方向进行了机制研究,结果表明不同 CGAs 亚组的吸收速率不同。我们首次证明了完整的咖啡酰奎尼酸和咖啡酰奎尼酸内酯通过胃上皮细胞的吸收(P(app)∼0.2 cm/s)。由于在孵育时间和测试浓度范围内观察到良好的线性关系,因此推测吸收可能主要通过被动扩散进行,我们推测潜在的载体介导成分可能参与某些 4-酰基 CGAs 异构体的摄取。相比之下,完整的二咖啡酰奎尼酸的吸收速度很快(P(app)∼2-10 cm/s),但与时间和浓度的依赖性呈非线性关系,这可能是由于与外排转运体的相互作用和/或 pH 梯度依赖性受到限制。本研究首次在胃黏膜中显示了绿原酸的甲基化。此外,异阿魏酸、二甲氧基肉桂酸和阿魏酸被鉴定为绿原酸生物转化的新型胃代谢物。我们提出胃是释放羟基肉桂酸的第一个部位,这可以解释为什么在喝咖啡后能很快检测到它们。

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