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酪氨酰-色氨酸-甲硫氨酰-异亮氨酰-苯丙氨酰-缬氨酰-甘氨酰胺-1(Tyr-W-MIF-1)可减轻SH-SY5Y人神经母细胞瘤细胞中阿片受体的下调。

Tyr-W-MIF-1 attenuates down-regulation of opiate receptors in SH-SY5Y human neuroblastoma cells.

作者信息

Harrison L M, Kastin A J, Zadina J E

机构信息

Tulane University School of Medicine and Veterans Affairs Medical Center, New Orleans, Louisiana 70146, USA.

出版信息

J Pharmacol Exp Ther. 1998 Feb;284(2):611-7.

PMID:9454805
Abstract

Down-regulation of opiate receptors is demonstrated more easily in vitro than in vivo. The possible role of endogenous opiate-modulating peptides in preventing such down-regulation was investigated by addition of Tyr-W-MIF-1 to an in vitro preparation, the human neuroblastoma cell line SH-SY5Y, in which down-regulation of opiate receptors has been demonstrated previously. Although both morphine and Met-enkephalin down-regulated mu and delta receptors after chronic (24 h) exposure in serum-free medium, Tyr-W-MIF-1, at doses of up to 100 microM, did not affect receptor number when administered alone. This lack of effect could not be attributed to degradation of the peptide during chronic treatment because high-performance liquid chromatography showed that 79% of the peptide remained intact after a 24-h incubation. When coadministered with 3 microM morphine, Tyr-W-MIF-1 dose-dependently attenuated morphine-induced down-regulation of both mu and delta receptors. Down-regulation of mu receptors by the selective agonist PL017 was also attenuated by Tyr-W-MIF-1, but down-regulation of delta receptors by the selective agonist DPDPE was not. These studies indicate that endogenous opiate modulators may play a role in opiate tolerance at the level of receptor down-regulation.

摘要

与体内相比,阿片受体的下调在体外更容易得到证实。通过将酪氨酰 -W-促黑素细胞激素释放抑制因子 -1(Tyr-W-MIF-1)添加到体外制备物——人神经母细胞瘤细胞系SH-SY5Y中,研究内源性阿片调节肽在预防此类下调中可能发挥的作用,此前已证实在该细胞系中存在阿片受体的下调。尽管在无血清培养基中慢性(24小时)暴露后,吗啡和甲硫氨酸脑啡肽均下调了μ和δ受体,但单独给予高达100微摩尔剂量的Tyr-W-MIF-1时,并未影响受体数量。这种无作用不能归因于慢性处理过程中该肽的降解,因为高效液相色谱显示,孵育24小时后,79%的肽仍保持完整。当与3微摩尔吗啡共同给药时,Tyr-W-MIF-1呈剂量依赖性地减弱吗啡诱导的μ和δ受体下调。选择性激动剂PL017诱导的μ受体下调也被Tyr-W-MIF-1减弱,但选择性激动剂DPDPE诱导的δ受体下调则未被减弱。这些研究表明,内源性阿片调节剂可能在受体下调水平的阿片耐受性中发挥作用。

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