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Functional characterization of tyrosine transport in fibroblast cells from healthy controls.

机译:来自健康对照的成纤维细胞中酪氨酸转运的功能表征。

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Human fibroblast cells are an advantageous model to study the transport of amino acids across cell membranes, since one can control the environmental factors. A major problem in all earlier studies is the lack of precise and detailed knowledge regarding the expression and functionality of tyrosine transporters in human fibroblasts. This motivated us to perform a systematic functional characterization of the tyrosine transport in fibroblast cells with respect to the isoforms of system-L (LAT1, LAT2, LAT3, LAT4), which is the major transporter of tyrosine. Ten (n=10) fibroblast cell lines from healthy volunteers were included in the study. Uptake of L-[U-14C] tyrosine in fibroblasts was measured using the cluster tray method in the presence and absence of excess concentrations of various combinations of inhibitors. This study demonstrated that LAT1 is involved in 90% of total uptake of tyrosine and also around 51% of alanine. Not more than 10% can be accounted for by LAT2, LAT3 and LAT4 isoforms. LAT2 seems to be functionally weak in uptake of tyrosine while LAT3 and LAT4 contributed around 7%. 10% could be contributed by system-A (ATA2 isoform). Alanine consequently inhibited the tyrosine transport by up to 60%. Tyrosine transport through the LAT1 isoform has a higher affinity compared to system-L. In conclusion, the LAT1 isoform is the major transporter of tyrosine in human fibroblast cells. Competition between tyrosine and alanine for transport is shown to exist, probably between LAT1 and LAT2 isoforms. This study established fibroblast cells as a suitable experimental model for studying amino acid transport defects in humans.
机译:人类成纤维细胞是研究氨基酸跨细胞膜运输的一种有利模型,因为它可以控制环境因素。所有早期研究的一个主要问题是缺乏关于人成纤维细胞中酪氨酸转运蛋白表达和功能的精确和详细的知识。这促使我们对成纤维细胞中酪氨酸转运系统L(LAT1,LAT2,LAT3,LAT4)的同工型进行系统的功能表征,后者是酪氨酸的主要转运体。来自健康志愿者的十个(n = 10)成纤维细胞系被纳入研究。在存在和不存在过量浓度的各种抑制剂组合的情况下,使用簇状托盘法测量了成纤维细胞中L- [U-14C]酪氨酸的摄取。这项研究表明,LAT1参与了90%的酪氨酸摄取,还参与了约51%的丙氨酸摄取。 LAT2,LAT3和LAT4异构体的含量不能超过10%。 LAT2似乎在功能上对酪氨酸的吸收较弱,而LAT3和LAT4的贡献约为7%。系统A(ATA2亚型)贡献了10%。因此,丙氨酸最多可抑制60%的酪氨酸转运。与L系统相比,通过LAT1同工型的酪氨酸转运具有更高的亲和力。总之,LAT1亚型是人类成纤维细胞中酪氨酸的主要转运蛋白。酪氨酸和丙氨酸之间存在运输竞争,很可能存在于LAT1和LAT2同工型之间。这项研究建立了成纤维细胞作为研究人体氨基酸转运缺陷的合适实验模型。

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