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视网膜色素上皮细胞中内源性阿片肽新型钠氯偶联转运系统的鉴定及HIV-1 Tat对该转运系统的诱导作用

Identification of a novel Na+- and Cl--coupled transport system for endogenous opioid peptides in retinal pigment epithelium and induction of the transport system by HIV-1 Tat.

作者信息

Hu Huankai, Miyauchi Seiji, Bridges Christy C, Smith Sylvia B, Ganapathy Vadivel

机构信息

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

出版信息

Biochem J. 2003 Oct 1;375(Pt 1):17-22. doi: 10.1042/BJ20031059.

DOI:10.1042/BJ20031059
PMID:12924983
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1223675/
Abstract

The endogenous opioid peptides enkephalins, dynorphins and endorphins consist of five or more amino acids. These peptides participate in a multitude of biological functions in mammalian cells by interacting with different subtypes of opiate receptors located on the plasma membrane and in the nucleus. Here we report on the identification of a new peptide transport system in the human retinal pigment epithelial (RPE) cells that transports a variety of endogenous opioid peptides with high affinity. We identified this novel, hitherto unrecognized, transport system when we were analysing the differential effects of Tat, the transacting factor encoded by HIV-1, on various transport processes in RPE cells. This transport system is markedly induced by Tat. This opioid transport system is energized by transmembrane Na+ and Cl- gradients and is distinct from any of the previously identified transport systems for opioid peptides in mammalian cells. Free amino acids, dipeptides, tripeptides and non-peptide opiate receptor antagonists are excluded by this newly identified transport system. The affinities of endogenous opioid peptides for this system are in the range of 0.4-40 microM. The identification of the high-affinity Na+- and Cl--coupled transport system in mammalian cells that is specific for endogenous opioid peptides and is induced by HIV-1 Tat is of significance not only to the biology of opioid peptides but also to the pathology of HIV-1 infection in humans.

摘要

内源性阿片肽脑啡肽、强啡肽和内啡肽由五个或更多氨基酸组成。这些肽通过与位于质膜和细胞核上的不同亚型阿片受体相互作用,参与哺乳动物细胞中的多种生物学功能。在此,我们报告在人视网膜色素上皮(RPE)细胞中鉴定出一种新的肽转运系统,该系统以高亲和力转运多种内源性阿片肽。当我们分析HIV-1编码的反式作用因子Tat对RPE细胞中各种转运过程的差异影响时,鉴定出了这种新颖的、迄今未被认识的转运系统。该转运系统由Tat显著诱导。这种阿片肽转运系统由跨膜Na⁺和Cl⁻梯度提供能量,并且不同于哺乳动物细胞中先前鉴定出的任何阿片肽转运系统。这种新鉴定出的转运系统排除了游离氨基酸、二肽、三肽和非肽类阿片受体拮抗剂。内源性阿片肽对该系统的亲和力在0.4 - 40微摩尔范围内。在哺乳动物细胞中鉴定出对内源性阿片肽具有特异性且由HIV-1 Tat诱导的高亲和力Na⁺和Cl⁻偶联转运系统,不仅对阿片肽生物学具有重要意义,而且对人类HIV-1感染病理学也具有重要意义。

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Exploring the opioid system by gene knockout.通过基因敲除探索阿片类系统。
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