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酪蛋白酸钠和维生素 A 络合对 Caco-2 细胞中维生素 A 的生物利用度和生物可及性的影响。

Effect of sodium caseinate and vitamin A complexation on bioaccessibility and bioavailability of vitamin A in Caco-2 cells.

机构信息

Dairy Chemistry Division, National Dairy Research Institute, Karnal, Haryana 132001, India.

Dairy Chemistry Division, National Dairy Research Institute, Karnal, Haryana 132001, India.

出版信息

Food Res Int. 2019 Jul;121:910-918. doi: 10.1016/j.foodres.2019.01.019. Epub 2019 Jan 11.

Abstract

Native sodium caseinate-vitamin A (VA) complexes (Sodium caseinate-VA complex, NaCaS-VA) and modified sodium caseinate-VA complexes i.e. Succinylated sodium caseinate-VA complex (SNaCaS-VA), reassembled sodium caseinate-VA complex (RNaCaS-VA) and reassembled succinylated sodium caseinate-VA complex (RSNaCaS-VA) were prepared and evaluated for their in-vitro bioaccessibility and in-vitro bioavailability of VA through Caco-2 cell lines.VA degraded under acidic conditions as the physiological pH during digestion in stomach was highly acidic (1.2-1.8). During in-vitro gastric digestion, sodium caseinate provided protection to VA, hence, higher VA content was retained in digesta as compared to free VA (oily form). Vitamin uptake by Caco-2 cells was significantly different for digested sodium caseinate-VA complexes as compared to free VA. The peptide content of casein and various sodium caseinate-VA complexes was monitored throughout digestion process. Variation in the complex composition had an effect on protein digestibility and peptide distribution. The bioavailability of VA through sodium caseinate-VA complexes was evaluated by exposing Caco-2 cells to the digesta of milk fortified with various complexes. The total uptake of VA by Caco-2 cells was highest for milk fortified with RSNaCaS-VA followed by RNaCaS-VA, control milk, SNaCaS-VA, NaCaS-VA and free VA. During the formation of RNaCaS-VA and RSNaCaS-VA complexes more hydrophobic sites are exposed, leading to the attachment of VA on the interior hydrophobic regions of sodium caseinate molecule. This led to higher stability of VA during gastrointestinal digestion and further resulted in higher bioaccessibility and bioavailability of vitamin A in Caco-2 cells.

摘要

天然酪蛋白 - 维生素 A(VA)复合物(酪蛋白酸钠 - VA 复合物,NaCaS-VA)和改性酪蛋白酸钠 - VA 复合物,即琥珀酰化酪蛋白酸钠 - VA 复合物(SNaCaS-VA)、重组酪蛋白酸钠 - VA 复合物(RNaCaS-VA)和重组琥珀酰化酪蛋白酸钠 - VA 复合物(RSNaCaS-VA)被制备并通过 Caco-2 细胞系评估其 VA 的体外生物利用度和体外生物可及性。VA 在酸性条件下降解,因为在胃中消化期间的生理 pH 值非常低(1.2-1.8)。在体外胃消化过程中,酪蛋白酸钠为 VA 提供了保护,因此,与游离 VA(油状形式)相比,更多的 VA 含量保留在消化物中。与游离 VA 相比,消化后的酪蛋白酸钠-VA 复合物对 Caco-2 细胞的 VA 吸收有显著差异。整个消化过程中监测了酪蛋白和各种酪蛋白酸钠-VA 复合物的肽含量。复合物组成的变化会影响蛋白质消化率和肽分布。通过将 Caco-2 细胞暴露于用各种复合物强化的牛奶消化物中来评估 VA 通过酪蛋白酸钠-VA 复合物的生物利用度。Caco-2 细胞对 VA 的总摄取量以添加 RSNaCaS-VA 的牛奶最高,其次是 RNaCaS-VA、对照牛奶、SNaCaS-VA、NaCaS-VA 和游离 VA。在 RNaCaS-VA 和 RSNaCaS-VA 复合物的形成过程中,更多的疏水区暴露,导致 VA 附着在酪蛋白酸钠分子的内部疏水区。这导致 VA 在胃肠道消化过程中更加稳定,进一步导致 Caco-2 细胞中维生素 A 的生物可及性和生物利用度更高。

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