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在用单胺氧化酶抑制剂预处理的豚鼠中,色胺诱导的肌阵挛表明色胺对中枢吲哚胺系统具有突触前和突触后作用。

Tryptamine-induced myoclonus in guinea-pigs pretreated with a monoamine oxidase inhibitor indicates pre- and post-synaptic actions of tryptamine upon central indoleamine systems.

作者信息

Luscombe G, Jenner P, Marsden C D

出版信息

Neuropharmacology. 1982 Dec;21(12):1257-65. doi: 10.1016/0028-3908(82)90130-7.

Abstract

Tryptamine (1-320 mg/kg) evoked only slight muscle jerking in naive guinea-pigs but, in animals pretreated with pargyline (75 mg/kg; 1 hr previously), tryptamine induced a dose-dependent (6-160 mg/kg) myoclonus. The myoclonus induced by tryptamine (40 mg/kg) plus pargyline (75 mg/kg) was differentially inhibited by the indoleamine receptor antagonists, methergoline (5 mg/kg) which was more potent than methysergide (10 mg/kg), mianserin (10 mg/kg) which was more potent that cyproheptadine (10 mg/kg) and propranolol (20 mg/kg) which was more potent than cinanserin (10 mg/kg). This rank order of potency differed from that observed for the order of potency of these drugs in inhibiting the myoclonus induced by L-5-hydroxytryptophan (5HTP) plus carbidopa in guinea-pigs (Luscombe, Jenner and Marsden, Neuropharmacology, 1981), perhaps indicating involvement of pharmacologically distinct indoleamine receptors. Manipulation of presynaptic function of 5-hydroxytryptamine (5HT) by tryptophan hydroxylase inhibition with p-chlorophenylalanine to produce depletion of cerebral 5HT, or by an L-tryptophan load to elevate 5HT in brain, suggested that the functional integrity of serotonergic neurones is required for the expression of myoclonus induced by tryptamine plus pargyline. A range of blockers of 5HT re-uptake did not alter the jerking produced by tryptamine (40 mg/kg) in guinea pigs pretreated with pargyline (75 mg/kg; 1 hr previously), or the threshold myoclonus induced by a smaller dose of tryptamine (10 mg/kg; plus pargyline 75 mg/kg). It is suggested that myoclonus induced by tryptamine in guinea pigs pretreated with pargyline involves activation of post-synaptic indoleamine receptors by tryptamine by a mechanism which requires intact presynaptic function of 5HT.

摘要

色胺(1 - 320毫克/千克)在未处理的豚鼠中仅引起轻微的肌肉抽搐,但在预先用优降宁(75毫克/千克;1小时前)处理的动物中,色胺诱导出剂量依赖性(6 - 160毫克/千克)的肌阵挛。色胺(40毫克/千克)加优降宁(75毫克/千克)诱导的肌阵挛被吲哚胺受体拮抗剂差异性抑制,麦角苄酯(5毫克/千克)比甲基麦角新碱(10毫克/千克)更有效,米安色林(10毫克/千克)比赛庚啶(10毫克/千克)更有效,普萘洛尔(20毫克/千克)比辛那色林(10毫克/千克)更有效。这种效价顺序与这些药物在抑制豚鼠中L - 5 - 羟色氨酸(5HTP)加卡比多巴诱导的肌阵挛时观察到的效价顺序不同(卢斯科姆、詹纳和马斯登,《神经药理学》,1981年),这可能表明涉及药理学上不同的吲哚胺受体。通过用对氯苯丙氨酸抑制色氨酸羟化酶以耗尽脑内5HT来操纵5 - 羟色胺(5HT)的突触前功能,或通过给予L - 色氨酸负荷以提高脑内5HT,表明5HT能神经元的功能完整性是色胺加优降宁诱导的肌阵挛表达所必需的。一系列5HT再摄取阻滞剂并未改变在用优降宁(75毫克/千克;1小时前)预处理的豚鼠中色胺(40毫克/千克)产生的抽搐,或较小剂量色胺(10毫克/千克;加优降宁75毫克/千克)诱导的阈下肌阵挛。有人提出,在用优降宁预处理的豚鼠中,色胺诱导的肌阵挛涉及色胺通过一种需要5HT完整突触前功能的机制激活突触后吲哚胺受体。

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