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首页> 外文期刊>American Journal of Physiology >Expression of the reduced folate carrier SLC19A1 in IEC-6 cells results in two distinct transport activities.
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Expression of the reduced folate carrier SLC19A1 in IEC-6 cells results in two distinct transport activities.

机译:还原的叶酸载体SLC19A1在IEC-6细胞中的表达导致两种不同的转运活性。

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Intestinal absorption of folates has been characterized as a facilitative process with a low pH optimum. Studies with intestinal epithelial cells have suggested that this activity is mediated by the reduced folate carrier (RFC1). In this paper, we report on folate transport characteristics in an immortalized rat IEC-6 cell line that was found to exhibit the predominant influx activity for methotrexate (MTX) at pH 5.5 with a low level of activity at pH 7.4. Transfection of this cell line with an RFC1 construct resulted in clones exhibiting increased MTX uptake at both the pHs and high folic acid uptake only at the low pH. For the two clones with the highest level of transport activity, relative MTX influx at the two pHs was reversed. Moreover, the low pH MTX influx activity ([MTX](e) = 0.5 microM) was markedly inhibited by 20 microM folic acid while influx at neutral pH was not. Furthermore, in the presence and absence of glucose at low pH, MTX and folic acid influx activity was inhibited by azide, while MTX influx at pH 7.4 was stimulated by azide in the absence of glucose but was unchanged in the presence of glucose and azide. This was contrasted with the results of transfection of the same RFC1 construct into an L1210 murine leukemia cell line bearing a nonfunctional endogenous carrier. In this case, the activity expressed was only at pH 7.4. These data indicate that RFC1 can exhibit two distinct types of folate transport activities in intestinal cells that must depend on tissue-specific modulators.
机译:叶酸在肠中的吸收被认为是pH值较低的促进过程。对肠道上皮细胞的研究表明,这种活性是由减少的叶酸载体(RFC1)介导的。在本文中,我们报告了永生化大鼠IEC-6细胞系中的叶酸转运特性,该细胞系在pH 5.5时表现出对甲氨蝶呤(MTX)的主要流入活性,在pH 7.4时表现出低水平的活性。用RFC1构建体转染该细胞系会导致克隆在pH值下均显示MTX摄取增加,而仅在低pH值时显示高叶酸摄取。对于具有最高运输活性水平的两个克隆,在两个pH处的相对MTX流入被逆转。此外,低pH值MTX流入活性([MTX](e)= 0.5 microM)被20 microM叶酸显着抑制,而中性pH则没有。此外,在低pH下存在和不存在葡萄糖的情况下,叠氮化物抑制了MTX和叶酸的流入活性,而在不存在葡萄糖的情况下,叠氮化物刺激了pH 7.4的MTX流入,但是在存在葡萄糖和叠氮化物的情况下保持不变。这与将相同RFC1构建体转染到带有非功能性内源性载体的L1210鼠白血病细胞系中的结果形成对比。在这种情况下,所表达的活性仅在pH 7.4下。这些数据表明,RFC1在肠道细胞中可表现出两种不同类型的叶酸转运活性,这必须依赖于组织特异性调节剂。

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