胍丁胺抑制小鼠吗啡戒断与其抑制一氧化氮合酶的关系(英文)

Correlation between inhibitions of morphine withdrawal and nitric-oxide synthase by agmatine

目的:观察胍丁胺抑制纳洛酮引起小鼠吗啡戒断跳跃与其抑制一氧化氮合酶(NOS)的关系,方法:用测定[~3H]胍氨酸浓度的方法确定NOS活性,结果:在体外胍丁胺底物竞争性抑制正常和吗啡依赖小鼠小脑、端脑和丘脑NOS活性,纳洛酮引起吗啡依赖小鼠戒断跳跃和小脑、端脑、丘脑NOS活性升高,用吗啡和胍丁胺共同处理小鼠显著抑制纳洛酮促使小鼠戒断跳跃和NOS活性升高的作用,咪唑克生抑制胍丁胺的此作用,结论:胍丁胺对纳洛酮引起戒断跳跃的抑制作用与其通过激活咪唑啉受体和底物竞争性抑制NOS活性相关。

AIM: To study correlation between inhibitions of naloxone-precipitated withdrawal jumps and nitric-oxide synthase (NOS) activity by agmatine. METHODS: NOS activities in mouse brain were measured by determination of concentration of [3H]citrulline, the product of [3H]arginine. RESULTS: Agmatine inhibited NOS activity in naive and morphine-dependent mouse cerebellum, forebrain, and thalamus in substrate-competitive manner in vitro. Naloxone induced withdrawal jumps and an increase in NOS activity in cerebellum, forebrain, and thalamus of abstinent mice. Pretreatment of mice with morphine plus agmatine inhibited the effect of naloxone to precipitate withdrawal jumps and increase in NOS activity. The effect of agmatine was blocked by idazoxan. CONCLUSION: The inhibitory effect of agmatine on naloxone-precipitated withdrawal jumps is related to its inhibition of NOS activity by substrate competitive manner and activation of imidazoline receptors.