胆碱并入磷脂酰胆碱与吗啡结合位点的关系。

R Natsuki
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引用次数: 0

摘要

研究了钙(25 mM)刺激胆碱并入磷脂酰胆碱(PC)和3h -吗啡(3H-M)结合,使用急性吗啡治疗小鼠、吗啡依赖小鼠和吗啡戒断小鼠的脑粗突触体部分。老鼠在摄入含有吗啡的食物后对吗啡产生了生理依赖。吗啡依赖抑制14c -胆碱向PC的掺入。吗啡依赖小鼠注射纳洛酮(1 mg/kg)也能抑制14c -胆碱向PC的掺入。吗啡戒断小鼠注射吗啡(10 mg/kg)可刺激14c -胆碱并入PC,但对急性吗啡治疗小鼠和吗啡依赖小鼠均无影响。纳洛酮(1 mg/kg)、吗啡(10 mg/kg)、吗啡依赖和阿片类戒断(最后一次从食物中接触吗啡20小时后)均导致小鼠脑突触体3H-M (10(-7) M)结合减少约25%。在死亡前45分钟注射10 mg/kg吗啡可使依赖小鼠和戒断小鼠的3h -吗啡结合再降低20%,而在幼稚小鼠中没有。对3H-M立体特异性结合(SSB)进行评价:1)体内纳洛酮对3H-M体外结合的影响,2)体内吗啡对3H-M体外结合的影响;3) 3H-M结合(体外)与纳洛酮和吗啡治疗(体内)的差异。吗啡戒断小鼠SSB活性高。这些差异可能是由与耐受性和戒断相关的阿片受体的变化引起的,也可能发生在PC和膜受体之间。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Relationship between incorporation of choline into phosphatidylcholine and morphine binding sites.

Calcium (25 mM)-stimulated incorporation of choline into phosphatidylcholine (PC) and 3H-morphine (3H-M) binding was studied using cerebral crude synaptosomal fractions from acute morphine-treated (naive), morphine-dependent and morphine-withdrawn mice. Mice became physically dependent on morphine after ingesting morphine-mixed food. Morphine dependence inhibited the incorporation of 14C-choline into PC. The injection of naloxone (1 mg/kg) to morphine-dependent mice also inhibited the incorporation of 14C-choline into PC. The injection of morphine (10 mg/kg) to morphine-withdrawn mice stimulated the incorporation of 14C-choline into PC, but had no effect, either on acute morphine-treated mice or on morphine-dependent mice. Naloxone (1 mg/kg), morphine (10 mg/kg), morphine dependence and opiate withdrawal (20 hrs after the last exposure to morphine in food) all caused about a 25% decrease in 3H-M (10(-7) M) binding to mouse brain synaptosomes. The injection of 10 mg/kg of morphine 45 min before death caused an additional 20% decrease in 3H-morphine binding in the dependent and withdrawn mice, but not in the naive mice. Stereospecific binding (SSB) of 3H-M was evaluated with respect to: 1) the effect of naloxone treatment in vivo on 3H-M binding in vitro, 2) the effect of morphine treatment in vivo on 3H-M binding in vitro; and 3) the differences between 3H-M bound (in vitro) and both naloxone and morphine treatment (in vivo). SSB activity was high in morphine-withdrawn mice. These differences may be caused by changes in the opiate receptors related to tolerance and withdrawal, and may entail between PC and membrane receptors.

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