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一种新型的 Caco-2 体外肠道屏障细胞模型:用于评估镁盐吸收的应用。

A New Caco-2 Cell Model of in Vitro Intestinal Barrier: Application for the Evaluation of Magnesium Salts Absorption.

机构信息

Faculty of Medicine, Comenius University Bratislava, Institute of Pharmacology and Clinical Pharmacology, Bratislava, Slovakia.

出版信息

Physiol Res. 2021 Nov 30;70(Suppl 1):S31-S41.

Abstract

Experimental data concerning the bioavailability of the different Mg-salts in human organism is inconsistent. Mg-absorption reported by clinical studies largely varies depending on the method used for evaluation. The aim of this study was to evaluate the bioavailability and accessibility of magnesium bound in different Mg-salt compounds, using an in vitro model of intestinal cell barrier. The study included a variety of inorganic (oxide, sulphate, chloride, carbonate) and organic salts (lactate, citrate, pidolate). Caco-2 cells were cultivated in a complete culture medium with different magnesium salts treatments in ascending concentrations. The viability and quantity of cells was analysed by FACS. Mg-absorption was analysed by a direct colorimetric assay, measured by spectrometry. T-test identified a significant decrease in cell count treatment with mg-lactate compared with citrate. Mg-pidolate showed a significantly higher cell viability compared with Mg-citrate, Mg-lactate and Mg-chloride. Even though the difference was not significant, we showed that an increase in Mg2+ salt concentration progressively decreased the cell count and the viability and the effect was universal for all the used Mg-salt treatments. Mg-citrate, chloride, and sulphate showed a significantly lower absorption compared to Mg-carbonate, pidolate and oxide. Our in vitro monolayer model of human intestinal transport showed that viability and quantity of cell decreased with increasing Mg-concentration. We admit that our experiment model may have some limitations in accurately describing an in vivo Mg2+ absorption. Moreover, it is also necessary to assess the relevance of our data in vivo and especially in clinical practice.

摘要

关于不同镁盐在人体中的生物利用度的实验数据不一致。临床研究报告的镁吸收率在很大程度上取决于用于评估的方法。本研究旨在使用肠细胞屏障的体外模型评估不同镁盐化合物结合的镁的生物利用度和可及性。该研究包括各种无机(氧化物、硫酸盐、氯化物、碳酸盐)和有机盐(乳酸盐、柠檬酸盐、丙二酸盐)。Caco-2 细胞在含有不同镁盐处理的完全培养基中培养,浓度逐渐升高。通过流式细胞术分析细胞活力和数量。通过直接比色法分析镁吸收,通过光谱法测量。T 检验确定与柠檬酸盐相比,用镁乳酸盐处理的细胞计数明显减少。与镁柠檬酸盐、镁乳酸盐和镁氯化物相比,镁丙二酸盐显示出更高的细胞活力。尽管差异不显著,但我们表明,随着 Mg2+盐浓度的增加,细胞计数和活力逐渐降低,这种效应对所有使用的 Mg 盐处理都是普遍的。与 Mg 碳酸盐、丙二酸盐和氧化物相比,镁柠檬酸盐、氯化物和硫酸盐的吸收明显较低。我们的人类肠转运体外单层模型表明,随着镁浓度的增加,细胞活力和数量减少。我们承认,我们的实验模型可能在准确描述体内 Mg2+吸收方面存在一些限制。此外,还需要评估我们的数据在体内特别是在临床实践中的相关性。

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