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在黑质内注射6-羟基多巴胺后14天,苯丙胺诱发的旋转需要新合成的多巴胺,但1天时则不需要,并且它始终与感觉运动行为分离。

Amphetamine-evoked rotation requires newly synthesized dopamine at 14 days but not 1 day after intranigral 6-OHDA and is consistently dissociated from sensorimotor behavior.

作者信息

Paquette Melanie A, Marsh Steven T, Hutchings Janet E, Castañeda Eddie

机构信息

Department of Psychology, Arizona State University, Tempe, AZ 85287-1104, USA.

出版信息

Behav Brain Res. 2009 Jun 8;200(1):197-207. doi: 10.1016/j.bbr.2009.01.017.

Abstract

Immediately after unilateral, intranigral 6-hydroxydopamine (6-OHDA), amphetamine (AMPH) evokes "paradoxical" contraversive rotation, whereas 14 days later, AMPH evokes the traditional ipsiversive rotation used to model the chronic Parkinsonian state. In this study, the hypothesis was that accelerated dopamine (DA) synthesis ipsilateral to the lesion augments cytoplasmic DA to produce paradoxical rotation. Therefore, the sensitivity to synthesis inhibition of AMPH-evoked rotation at 1 or 14 days after 6-OHDA was assessed. To determine the functional status that might be reflected by paradoxical rotation, sensorimotor abilities were examined at 1 and 14 days following unilateral 6-OHDA using the elevated swing, paw placement, grip strength, ladder walking, somatosensory neglect, and cylinder tests. At 14 days after 6-OHDA when AMPH-evoked ipsiversive rotation is mediated by the intact hemisphere, rotation was dose-dependently reduced by tyrosine hydroxylase (TH) inhibition with alpha-methyl-p-tyrosine (alpha-MPT) or dopa decarboxylase (DDC) inhibition with 3-hydroxybenzyl hydrazine (NSD-1015), indicating dependence upon newly synthesized DA. Conversely, at 1 day after 6-OHDA, paradoxical rotation, presumably mediated by the treated hemisphere, was completely resistant to synthesis blockade, indicating an abundant supply of intracellular DA that is independent from synthesis rates. Sensorimotor behaviors were not correlated with AMPH-evoked rotation. The present data do not support the hypothesis that enhanced DA synthesis is required to express paradoxical rotation. Therefore, alternative mechanisms that may enhance cytoplasmic DA to produce paradoxical rotation are discussed.

摘要

在单侧黑质内注射6-羟基多巴胺(6-OHDA)后立即给予苯丙胺(AMPH),会引发“反常”的向对侧旋转,而14天后,AMPH则会引发传统的向同侧旋转,用于模拟慢性帕金森状态。在本研究中,假设是损伤同侧多巴胺(DA)合成加速会增加细胞质DA以产生反常旋转。因此,评估了6-OHDA后1天或14天AMPH诱发旋转对合成抑制的敏感性。为了确定反常旋转可能反映的功能状态,在单侧6-OHDA后1天和14天,使用高架摆动、爪放置、握力、阶梯行走、体感忽视和圆柱体测试来检查感觉运动能力。在6-OHDA后14天,当AMPH诱发的向同侧旋转由完整半球介导时,用α-甲基-p-酪氨酸(α-MPT)抑制酪氨酸羟化酶(TH)或用3-羟基苄基肼(NSD-1015)抑制多巴脱羧酶(DDC)会使旋转剂量依赖性降低,表明依赖于新合成的DA。相反,在6-OHDA后1天,可能由处理过的半球介导的反常旋转对合成阻断完全有抗性,表明细胞内DA供应充足,与合成速率无关。感觉运动行为与AMPH诱发的旋转无关。目前的数据不支持增强DA合成是表达反常旋转所必需的这一假设。因此,讨论了可能增强细胞质DA以产生反常旋转的替代机制。

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