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小的非阿片肽和游离氨基酸对钠和氯依赖性阿片肽转运系统的差异调节作用。

Differential modulation of sodium- and chloride-dependent opioid peptide transport system by small nonopioid peptides and free amino acids.

作者信息

Miyauchi Seiji, Gopal Elangovan, Thakkar Santosh V, Ichikawa Satoshi, Prasad Puttur D, Ganapathy Vadivel

机构信息

Department of Biochemistry and Molecular Biology, Medical College of Georgia, Augusta, GA 30912, USA.

出版信息

J Pharmacol Exp Ther. 2007 Apr;321(1):257-64. doi: 10.1124/jpet.106.116806. Epub 2007 Jan 26.

Abstract

We recently identified a novel opioid peptide transport system in the retinal pigment epithelium that transports opioid peptides by a Na+/Cl--dependent process. Here we describe a similar transport system expressed in SK-N-SH cells (a human neuronal cell line) and show for the first time that the activity of the transport system is modulated differentially by lysine and small nonopioid peptides. The transport process in SK-N-SH cells, monitored with deltorphin II as the substrate, is Na+/Cl--dependent and interacts with several opioid peptides, consisting of 5 to 13 amino acids. The activity of this transport system is markedly stimulated by specific dipeptides and tripeptides, with significant stimulation observable at low micromolar concentrations. The ion dependence, Na+/Cl--activation kinetics, and opioid peptide selectivity of the transport system, however, remain unchanged. The stimulation by the modulatory peptides is associated with an increase in maximal velocity with no change in substrate affinity of the system. Amino acids have no or little effect on the transport system, with the exception of lysine. This cationic amino acid inhibits the transport system, with significant inhibition occurring at physiologic concentrations of the amino acid. The inhibitory effect is primarily associated with a decrease in the maximal velocity of the transport system with little change in substrate affinity. Methyl and ethyl esters of lysine retain the inhibitory potency, but most other structural analogs have no effect. The differential modulation of the transport system by lysine and specific small peptides has important implications in the biology and pharmacology of opioid peptides.

摘要

我们最近在视网膜色素上皮细胞中发现了一种新型阿片肽转运系统,该系统通过Na⁺/Cl⁻依赖性过程转运阿片肽。在此,我们描述了一种在SK-N-SH细胞(一种人神经细胞系)中表达的类似转运系统,并首次表明该转运系统的活性受到赖氨酸和小分子非阿片肽的不同调节。以强啡肽II为底物监测SK-N-SH细胞中的转运过程,该过程是Na⁺/Cl⁻依赖性的,并且与几种由5至13个氨基酸组成的阿片肽相互作用。该转运系统的活性受到特定二肽和三肽的显著刺激,在低微摩尔浓度下即可观察到明显的刺激作用。然而,该转运系统的离子依赖性、Na⁺/Cl⁻激活动力学和阿片肽选择性保持不变。调节肽的刺激与最大速度的增加相关,而系统的底物亲和力没有变化。氨基酸对转运系统没有影响或影响很小,但赖氨酸除外。这种阳离子氨基酸抑制转运系统,在氨基酸的生理浓度下即可发生显著抑制。抑制作用主要与转运系统最大速度的降低相关,而底物亲和力变化不大。赖氨酸的甲酯和乙酯保留了抑制效力,但大多数其他结构类似物没有作用。赖氨酸和特定小肽对转运系统的不同调节对阿片肽的生物学和药理学具有重要意义。

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