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首页> 外文期刊>British Journal of Pharmacology >A comparative study on the acute and long-term effects of MDMA and 3,4-dihydroxymethamphetamine (HHMA) on brain monoamine levels after i.p. or striatal administration in mice
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A comparative study on the acute and long-term effects of MDMA and 3,4-dihydroxymethamphetamine (HHMA) on brain monoamine levels after i.p. or striatal administration in mice

机译:腹腔注射后MDMA和3,4-二羟基甲基苯丙胺(HHMA)对脑单胺水平的急性和长期作用的比较研究或小鼠纹状体给药

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1 This study investigated whether the immediate and long-term effects of 3,4-methylenedioxy-methamphetamine (MDMA) on monoamines in mouse brain are due to the parent compound and the possible contribution of a major reactive metabolite, 3,4-dihydroxymethamphetamine (HHMA), to these changes. The acute effect of each compound on rectal temperature was also determined. 2 MDMA given i.p. (30 mg kg~(-1), three times at 3-h intervals), but not into the striatum (1, 10 and 100 μg, three times at 3-h intervals), produced a reduction in striatal dopamine content and modest 5-HT reduction 1 h after the last dose. MDMA does not therefore appear to be responsible for the acute monoamine release that follows its peripheral injection. 3 HHMA does not contribute to the acute MDMA-induced dopamine depletion as the acute central effects of MDMA and HHMA differed following i.p. injection. Both compounds induced hyperthermia, confirming that the acute dopamine depletion is not responsible for the temperature changes. 4 Peripheral administration of MDMA produced dopamine depletion 7 days later. Intrastriatal MDMA administration only produced a long-term loss of dopamine at much higher concentrations than those reached after the i.p. dose and therefore bears little relevance to the neurotoxicity. This indicates that the long-term effect is not attributable to the parent compound. HHMA also appeared not to be responsible as i.p. administration failed to alter the striatal dopamine concentration 7 days later. 5 HHMA was detected in plasma, but not in brain, following MDMA (i.p.), but it can cross the blood-brain barrier as it was detected in the brain following its peripheral injection. 6 The fact that the acute changes induced by i.p. or intrastriatal HHMA administration differed indicates that HHMA is metabolised to other compounds which are responsible for changes observed after i.p. administration.
机译:1这项研究调查了3,4-亚甲基二氧基甲基苯丙胺(MDMA)对小鼠脑中单胺的近期和长期影响是否归因于母体化合物以及主要的反应性代谢物3,4-二羟基甲基苯丙胺( HHMA),以进行这些更改。还确定了每种化合物对直肠温度的急性作用。给定2 MDMA (30 mg kg〜(-1),每3小时间隔3次),但未进入纹状体(1、10和100μg,每3小时间隔3次),导致纹状体多巴胺含量降低,且适度最后一剂后1小时降低5-HT。因此,MDMA似乎不负责其外围注射后的急性单胺释放。 3 HHMA对急性MDMA诱导的多巴胺耗竭没有贡献,因为MDMA和HHMA的急性中枢作用在开腹后有所不同。注射。两种化合物均会引起体温过高,从而证实急性多巴胺消耗与温度变化无关。 4于7天后对MDMA进行外围给药会产生多巴胺消耗。纹状体内MDMA给药仅产生长期多巴胺流失,其浓度远高于腹膜内注射后达到的浓度。剂量,因此与神经毒性几乎没有关系。这表明长期作用不归因于母体化合物。 HHMA也似乎不负责i.p.给药7天后未能改变纹状体多巴胺浓度。 5 MDMA(i.p.)后在血浆中检测到HHMA,但在大脑中未检测到,但是它可以穿过血脑屏障,因为在外周注射后在大脑中检测到了HHMA。 6 i.p.引起的急性变化纹状体内或纹状体内注射HHMA的方式不同,表明HHMA被代谢为其他化合物,这些化合物负责在腹腔内注射后观察到的变化。管理。

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