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Tryptophan Transport in Human Fibroblast Cells—A Functional Characterization

机译:人成纤维细胞中的色氨酸转运—功能表征

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摘要

There are indications that serotonergic neurotransmission is disturbed in several psychiatric disorders. One explanation may be disturbed transport of tryptophan (precursor for serotonin synthesis) across cell membranes. Human fibroblast cells offer an advantageous model to study the transport of amino acids across cell membranes, since they are easy to propagate and the environmental factors can be controlled. The aim of this study was to functionally characterize tryptophan transport and to identify the main transporters of tryptophan in fibroblast cell lines from healthy controls.Tryptophan kinetic parameters (Vmax and Km) at low and high concentrations were measured in fibroblasts using the cluster tray method. Uptake of 3H (5)-L-tryptophan at different concentrations in the presence and absence of excess concentrations of inhibitors or combinations of inhibitors of amino acid transporters were also measured. Tryptophan transport at high concentration (0.5 mM) had low affinity and high Vmax and the LAT1 isoform of system-L was responsible for approximately 40% of the total uptake of tryptophan. In comparison, tryptophan transport at low concentration (50 nM) had higher affinity, lower Vmax and approximately 80% of tryptophan uptake was transported by system-L with LAT1 as the major isoform. The uptake of tryptophan at the low concentration was mainly sodium (Na+) dependent, while uptake at high substrate concentration was mainly Na+ independent. A series of different transporter inhibitors had varying inhibitory effects on tryptophan uptake.This study indicates that tryptophan is transported by multiple transporters that are active at different substrate concentrations in human fibroblast cells. The tryptophan transport trough system-L was mainly facilitated by the LAT1 isoform, at both low and high substrate concentrations of tryptophan.
机译:有迹象表明,在几种精神疾病中,血清素能神经传递受到干扰。一种解释可能是色氨酸(5-羟色胺合成的前体)跨细胞膜的运输受到干扰。人类成纤维细胞提供了一种有利的模型来研究氨基酸跨细胞膜的运输,因为它们易于繁殖并且可以控制环境因素。这项研究的目的是在功能上表征色氨酸的转运,并从健康对照中鉴定成纤维细胞系中色氨酸的主要转运蛋白。使用簇盘法测量成纤维细胞在低浓度和高浓度下的色氨酸动力学参数(Vmax和Km)。还测量了在存在和不存在过量浓度的氨基酸转运蛋白抑制剂或抑制剂组合的情况下,不同浓度的 3 H(5)-L-色氨酸的吸收。高浓度(0.5 mM)的色氨酸转运具有较低的亲和力和较高的Vmax,系统L的LAT1同工型约占色氨酸总摄入量的40%。相比之下,低浓度(50 nM)的色氨酸转运具有更高的亲和力,更低的Vmax,并且系统L以LAT1作为主要同工型转运了大约80%的色氨酸摄取。低浓度色氨酸的吸收主要依赖于钠(Na + ),而底物浓度高时的吸收主要依赖于Na + 。一系列不同的转运蛋白抑制剂对色氨酸的吸收具有不同的抑制作用。这项研究表明,色氨酸是由多种转运蛋白转运的,这些转运蛋白在人成纤维细胞中具有不同的底物浓度。色氨酸低谷底物浓度时,LAT1亚型主要促进了色氨酸转运槽系统-L。

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