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前额叶皮质的兴奋性毒性损伤通过反复激活神经降压素受体减弱了苯丙胺诱导的运动增强。

Excitotoxic lesions of the prefrontal cortex attenuate the potentiation of amphetamine-induced locomotion by repeated neurotensin receptor activation.

作者信息

Blackburn Annie, Dewar Karen, Bauco Pat, Rompré Pierre-Paul

机构信息

Centre de recherche Fernand-Seguin, Hôpital Louis-H. Lafontaine, 7331, Hochelaga, Montréal, Québec, Canada H1N 3V2.

出版信息

Brain Res. 2004 Feb 20;998(2):184-93. doi: 10.1016/j.brainres.2003.11.022.

Abstract

This study was aimed at determining the role of prefrontal cortex neurons in the development of the potentiation of amphetamine-induced locomotor activity by repeated central injections of D-Tyr[11]neurotensin. Excitotoxic lesions of the prefrontal cortex were made by injecting bilaterally at three anterior-posterior placements 2 microg/microl of ibotenic acid. Ten days after surgery, locomotor responses to an intracerebroventricular injection of 0.18 or 18 nmol/10 microl of D-Tyr[11]neurotensin, or vehicle-saline, were measured in different groups of lesioned and sham rats. Ambulatory, non-ambulatory and vertical movements were measured for 2 h in activity cages starting immediately after the injection. This training phase was repeated on four occasions, every second day. One week after the last day of the training phase (day 14), locomotor responses to a single injection of amphetamine (0.75 mg/kg, IP) were measured in all rats. Results show that D-Tyr[11]neurotensin produced in sham animals a dose-dependent initial suppression of locomotor activity followed by an augmentation. The latter behavioral effect tended to be smaller in the lesioned rats, but not statistically different than in sham, suggesting that prefrontal cortex neurons do not play a major role in the stimulant effect of neurotensin on locomotor activity. However, sham rats pre-exposed to the high dose of D-Tyr[11]neurotensin showed stronger non-ambulatory and vertical movements than saline pre-exposed rats when tested with amphetamine; this sensitization effect was not observed in lesioned rats. The present results show that prefrontal cortex neurons are part of the neural circuitry involved in the development of amphetamine sensitization by repeated activation of central neurotensin receptors.

摘要

本研究旨在确定前额叶皮质神经元在通过反复向中枢注射D-Tyr[11]神经降压素增强苯丙胺诱导的运动活性过程中所起的作用。通过在三个前后位置双侧注射2微克/微升的鹅膏蕈氨酸来造成前额叶皮质的兴奋性毒性损伤。术后10天,在不同组的损伤大鼠和假手术大鼠中测量对脑室内注射0.18或18纳摩尔/10微升D-Tyr[11]神经降压素或溶剂生理盐水的运动反应。注射后立即在活动笼中测量2小时的行走、非行走和垂直运动。这个训练阶段每隔一天重复四次。在训练阶段的最后一天(第14天)之后一周,测量所有大鼠对单次注射苯丙胺(0.75毫克/千克,腹腔注射)的运动反应。结果表明,在假手术动物中,D-Tyr[11]神经降压素产生了剂量依赖性的初始运动活性抑制,随后是增强。后一种行为效应在损伤大鼠中往往较小,但与假手术大鼠相比无统计学差异,这表明前额叶皮质神经元在神经降压素对运动活性的刺激作用中不起主要作用。然而,预先暴露于高剂量D-Tyr[11]神经降压素的假手术大鼠在用苯丙胺测试时比预先暴露于生理盐水的大鼠表现出更强的非行走和垂直运动;在损伤大鼠中未观察到这种敏化效应。目前的结果表明,前额叶皮质神经元是通过中枢神经降压素受体的反复激活参与苯丙胺敏化发展的神经回路的一部分。

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