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Forelimb akinesia in the rat Parkinson model: differential effects of dopamine agonists and nigral transplants as assessed by a new stepping test

机译:大鼠帕金森病模型中的前肢运动障碍:通过新的步进测试评估多巴胺激动剂和黑色素移植物的差异作用

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摘要

Methods for the assessment of akinesia in the unilateral rat Parkinson model have so far been lacking. The experiments reported here evaluate the usefulness of a new “stepping test” to monitor forelimb akinesia in rats with unilateral 6-hydroxydopamine (6-OHDA) lesions of the mesencephalic dopamine (DA) system, and to assess the ability of DA- receptor agonists and fetal DA neuron transplants to reverse these deficits. The 6-OHDA lesion induced marked and long-lasting impairments in the initiation of stepping movements with the contralateral paw. Systemic injections of low doses (chosen to be subthreshold for induction of rotation) of the mixed D1 and D2 receptor agonist apomorphine, the D1-selective agonist SKF 38393, and to a lesser extent also the D2-selective agonist quinpirole were effective in reversing these deficits. Similar effects was seen after a subrotational dose of L-dopa, whereas amphetamine had no effect. Fetal nigral transplants, implanted as multiple deposits in the ipsilateral caudate-putamen and substantia nigra, restored initiation of stepping to a similar degree as the DA agonists. Nigral grafts placed in substantia nigra alone were also effective, although the improvement was less pronounced. Apomorphine, at a dose effective in the lesion-only animals, had no additive effect in the grafted rats, whereas amphetamine appeared to further improve stepping in the rats with intranigral transplants. Identical experiments were performed on skilled forelimb use in the so- called staircase test. Interestingly, neither the DA agonist drugs nor the nigral transplants had any effects on the lesion induced deficits in this more complex task. The results show that forelimb stepping is a highly useful test to monitor lesion-/and transplant-induced changes in forelimb akinesia, a behavioral parameter that may be analogous to limb akinesia and gait problems seen in patients with Parkinson's disease.
机译:迄今为止,尚缺乏用于评估单侧大鼠帕金森病模型中运动障碍的方法。此处报道的实验评估了新的“逐步测试”对监测中脑多巴胺(DA)系统单侧6-羟基多巴胺(6-OHDA)损伤的大鼠前肢运动障碍并评估DA受体激动剂的能力的有效性。和胎儿DA神经元移植来逆转这些缺陷。 6-OHDA病变在对侧脚掌开始踩踏运动时引起明显且持久的损伤。低剂量的全身性D1和D2受体激动剂阿扑吗啡,D1选择性激动剂SKF 38393以及较小程度的D2选择性激动剂喹吡罗的全身注射(选择低于诱导旋转的阈值)有效。赤字。亚旋转剂量的左旋多巴后可观察到类似效果,而苯丙胺则无作用。植入到同侧尾状丘脑和黑质中的多个沉积物的胎儿黑色移植物,恢复了开始步伐的程度与DA激动剂相似。尽管改善不那么明显,但仅将黑质植入黑质移植物中也是有效的。在仅病变动物中有效剂量的阿扑吗啡在移植的大鼠中没有加成作用,而苯丙胺似乎在进一步改善了经鼻移植的大鼠中的步伐。在熟练的前肢使用所谓的阶梯测试中进行了相同的实验。有趣的是,在这项更复杂的任务中,DA激动剂药物和黑色移植物均未对病变引起的缺陷产生任何影响。结果表明,前肢踩踏是监测病变/和移植引起的前肢运动障碍变化的非常有用的测试,该行为参数可能类似于帕金森氏病患者出现的肢体运动障碍和步态问题。

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