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星形胶质细胞中一种不依赖钠离子的中性氨基酸转运体对L-犬尿氨酸的高亲和力摄取。

High-affinity uptake of L-kynurenine by a Na+-independent transporter of neutral amino acids in astrocytes.

作者信息

Speciale C, Hares K, Schwarcz R, Brookes N

机构信息

Maryland Psychiatric Research Center, Baltimore 21228.

出版信息

J Neurosci. 1989 Jun;9(6):2066-72. doi: 10.1523/JNEUROSCI.09-06-02066.1989.

DOI:10.1523/JNEUROSCI.09-06-02066.1989
PMID:2723766
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6569713/
Abstract

L-Kynurenine (KYN), an intermediary product in the kynurenine pathway of tryptophan metabolism, is the common precursor from which are formed both quinolinic acid, a potent endogenous "excitotoxin," and kynurenic acid, a nonselective antagonist of excitotoxins. The present work examines 3H-KYN transport in primary astrocyte cultures derived from the cerebra of newborn mice. Influx and efflux of 3H-KYN were attributable almost entirely to carrier-mediated transport. The tritium recovered in uptake experiments was identifiable as 3H-KYN, indicating a low rate of KYN metabolism during incubations up to 30 min. KYN uptake decreased in the presence of extracellular Na+, at least in part because KYN efflux was accelerated. Marked trans stimulation of KYN efflux by extracellular KYN provided evidence of the exchanging nature of the carrier. Saturation curves for the initial velocity of KYN uptake conformed to a 1-component saturable system with Km of 32 microM and Vmax of 2.1 nmol mg-1 protein min-1. KYN was notably concentrated by the astrocytes, with an estimated steady-state distribution ratio of 180-fold for 1 microM KYN. Analog inhibition studies showed that the KYN transporter exhibited a clear preference for large neutral amino acids; leucine, tryptophan, and phenylalanine were recognized with relatively higher affinity than KYN. In summary, KYN is concentratively transported into astrocytes by a Na+-independent exchanger with high affinity for branched-chain and aromatic neutral amino acids. The substrate specificity and high affinity of this transport system resemble the properties of neutral amino acid transport across the blood-brain barrier in the rat and human.

摘要

L-犬尿氨酸(KYN)是色氨酸代谢犬尿氨酸途径中的一种中间产物,是强效内源性“兴奋性毒素”喹啉酸和兴奋性毒素的非选择性拮抗剂犬尿酸的共同前体。本研究检测了新生小鼠大脑来源的原代星形胶质细胞培养物中3H-KYN的转运。3H-KYN的流入和流出几乎完全归因于载体介导的转运。摄取实验中回收的氚可鉴定为3H-KYN,表明在长达30分钟的孵育过程中KYN代谢率较低。细胞外Na+存在时KYN摄取减少,至少部分原因是KYN流出加速。细胞外KYN对KYN流出有明显的反式刺激作用,证明了载体的交换性质。KYN摄取初始速度的饱和曲线符合单一组分可饱和系统,Km为32μM,Vmax为2.1 nmol mg-1蛋白min-1。星形胶质细胞显著浓缩KYN,对于1μM KYN,估计稳态分布比为180倍。类似物抑制研究表明,KYN转运体对大中性氨基酸有明显偏好;亮氨酸、色氨酸和苯丙氨酸比KYN具有相对更高的亲和力。总之,KYN通过对支链和芳香族中性氨基酸具有高亲和力的Na+非依赖性交换体被浓缩转运到星形胶质细胞中。该转运系统的底物特异性和高亲和力类似于大鼠和人类中跨血脑屏障的中性氨基酸转运特性。