摘要
目的:观察胍丁胺通过激活I1咪唑啉受体对阿片预处理引起的μ-阿片受体脱敏和下调的影响。方法:以CHO-μ和CHO-μ/IRAS(imidazoline receptor antisera-selected protein,咪唑啉受体抗血清选择性蛋白)细胞作为研究对象,用[35S]GTPγS和3H-二丙诺啡(diprenorphine)结合实验方法,确定胍丁胺-I1咪唑啉受体作用系统对μ-阿片受体脱敏和下调的影响。结果:在正常CHO-μ和CHO-μ/IRAS细胞中,μ-阿片受体的表达量和对配体的亲和力无显著差异;两细胞中μ-阿片受体对激动剂刺激的反应一致。阿片受体激动剂DAMGO[(D-Ala2,N-Me-Phe4,Gly5-ol)-脑啡肽(enkephalin),10μmol/L]处理CHO-μ/IRAS细胞30 minμ-阿片受体出现脱敏,而胍丁胺(10 nmol/L^100μmol/L)不影响μ-阿片受体脱敏过程。DAMGO(1μmol/L)处理两细胞12 h后可出现μ-阿片受体的下调,胍丁胺(1~100 nmol/L)浓度依赖性地抑制CHO-μ/IRAS细胞中μ-阿片受体的下调,而相同浓度胍丁胺在CHO-μ细胞中无此作用。胍丁胺这一作用能被I1咪唑啉受体阻断剂依法克生(efaroxan,Efa)所阻断。结论:胍丁胺通过激活I1咪唑啉受体可抑制DAMGO长期处理所致的μ-阿片受体下调,此作用可能与胍丁胺抑制阿片依赖有关。
Objective: To investigate the effects of agmatine by activation of I1 imidazoline receptor on DAMGO [ ( DAla^2 ,N-Me-Phe^4 ,Gly^5-ol)-enkephalin ]-induced desensitization and down-regulation of μ-opioid receptor. Methods: Two cell lines, Chinese hamster ovary cells expressing μ-opioid receptor alone ( CHO-μ) and co-expressing μ-opioid receptor and imidazoline receptor antisera-selected protein (IRAS), CHO-μ/IRAS i. e. a candidate for I1 imidazoline receptor, were used. [ 35↑S ] GTPγS binding assay and [ 3↑H ] diprenorphine binding assay were used to determine the effect on the desensitization and down-regulation of μ-opioid receptor by the agrnatine-I1 imidazoline receptor system. Results: There was no significant difference in expression and affinity of μ-opioid receptor between normal CHO-μ and CHO-Iμ /IRAS cells. The reaction of μ-opioid receptor in both cells was equal to the stimulation of ligand. DAMGO 10 μmol/L treatment for 30 min induced desensitization of μ-opioid receptor in CHO-μ/IRAS cells, while agmatine( 10 nmol/L - 10 μmol/L) did not influence DAMGO-induced desensitization of μ-opioid receptor. Chronic treatment with DAMGO ( 1 μmol/L, 12 h) decreased the expression of μ-opioid receptor in CHO-μ and CHO-μ/IRAS cells. Agmatine (1 -100 nM) concentration-dependently inhibited DAMGO-induced down-regulation of μ-opioid receptor in CHO-μ/IRAS cells, while this effect was not observed in CHO-μcells. Efaroxan, an I1 imidazoline receptor-preferential antagonist, completely reversed the effect of ag- matine in CHO-μ/IRAS cell. Conclusion: Agmatine could inhibit DAMGO-induced down-regulation of μ-opioid receptor by activation of I1 imidazoline receptor, which may contribute to the inhibition of opioid dependence by agmatine.
出处
《军事医学科学院院刊》
CSCD
北大核心
2007年第5期411-415,共5页
Bulletin of the Academy of Military Medical Sciences
基金
国家重点基础研究发展计划("973"计划)资助项目(2003CB515400)
关键词
胍丁胺
I1咪唑啉受体
Μ-阿片受体
脱敏
下调
agmatine
I1 imidazoline receptor
μ-opioid receptor
desensitization
down-regulation
