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首页> 外文期刊>Journal of Nutritional Science and Vitaminology >Cycloheximide treatment induces the uptake of neutral and dibasic amino acids via the activation of system b(0,+) in human intestinal Caco-2 cells.
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Cycloheximide treatment induces the uptake of neutral and dibasic amino acids via the activation of system b(0,+) in human intestinal Caco-2 cells.

机译:环己酰亚胺治疗通过激活人肠道Caco-2细胞中的系统b(0,+)诱导摄取中性和二价氨基酸。

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摘要

Amino acids in enterocytes are thought to be absorbed in the intestinal epithelium via various types of amino acid transport, although the regulation of these amino acid transport systems has not been elucidated. We examined in the present study the effect of several inhibitors involved in mRNA and protein synthesis, and of protein translocation on the L-leucine (Leu) uptake in human intestinal epithelial-like Caco-2 cells. Culturing Caco-2 cells with cycloheximide (CHX) enabled the L-Leu uptake to be significantly increased in a dose- and time-dependent manner. The uptake of L-lysine (Lys) was also increased by the CHX treatment, whereas the uptake of L-glutamate, taurine, and Gly-Gln was not changed. Among the two transport systems, b(0,+) and y+, which are known to be involved in L-Lys uptake by Caco-2, the system b(0,+) component was greatly increased by the CHX treatment, suggesting that system b(0,+) was mainly responsible for the increase in L-Leu and L-Lys uptake. The mRNA levels of rBAT and b(0,+) AT, whose molecules comprise system b(0,+), were both significantly increased by the CHX treatment in a time-dependent manner. These results strongly suggest that the CHX treatment increased the Leu and Lys uptake by activating system b(0,+) and inducing rBAT and b(0,+) AT mRNA expression in human intestinal epithelial Caco-2 cells.
机译:尽管尚未阐明对这些氨基酸转运系统的调节,但认为肠细胞中的氨基酸可通过各种类型的氨基酸转运被吸收到肠上皮中。我们在本研究中检查了几种抑制剂的参与mRNA和蛋白质合成,以及蛋白质易位对人肠上皮样Caco-2细胞L-亮氨酸(Leu)摄取的影响。用环己酰亚胺(CHX)培养Caco-2细胞可以使L-Leu摄取以剂量和时间依赖性方式显着增加。 CHX处理也增加了L-赖氨酸(Lys)的吸收,而L-谷氨酸,牛磺酸和Gly-Gln的吸收没有改变。在已知与Caco-2吸收L-Lys有关的两个转运系统b(0,+)和y +中,系统的b(0,+)成分通过CHX处理而大大增加,这表明系统b(0,+)主要负责L-Leu和L-Lys的摄取。分子组成系统b(0,+)的rBAT和b(0,+)AT的mRNA水平均通过CHX处理以时间依赖性方式显着增加。这些结果强烈表明,CHX处理通过激活系统b(0,+)并诱导人小肠上皮Caco-2细胞中的rBAT和b(0,+)AT mRNA表达来增加Leu和Lys摄取。

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