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帕金森病的实验性治疗

Experimental therapeutics of Parkinson's disease.

作者信息

Henderson Jasmine M

机构信息

Prince of Wales Medical Research Institute, Randwick, NSW, Australia.

出版信息

Clin Exp Pharmacol Physiol. 2003 Nov;30(11):841-4. doi: 10.1046/j.1440-1681.2003.03922.x.

Abstract
  1. The loss of central dopamine, which characterises Parkinson's disease, led to the main pharmacological strategy for treatment, namely levodopa, a dopamine-replacement therapy. Several years after treatment, the majority of patients experience dose-limiting side-effects and loss of symptom control. There is a resurgence of interest in neurosurgery for treating the Parkinson's disease, particularly in new techniques targeting the subthalamic nucleus (STN), which is overactive in Parkinson's disease and contributes to symptom development. 2. We performed unilateral subthalamotomy (lesioning the subthalamic nucleus via the toxin N-methyl-d-aspartate) in marmosets and rats with experimentally induced parkinsonism (induced using the toxin 6-hydroxydopamine). A range of similar behaviours common to both rodents and primates were evaluated before and after each type of surgery. Post-mortem histology was used to confirm the lesions. We also provide details of a case with Parkinson's disease who underwent high-frequency bilateral stimulation of the STN and in whom we analysed the STN post-mortem. 3. Unilateral subthalamotomy improved akinesia in parkinsonian primates. However, both monkeys and rodents showed postural abnormalities. The patient who underwent bilateral high-frequency stimulation showed improvement of akinesia and other disease symptoms and no postural abnormalities. Post-mortem analysis did not demonstrate substantial damage of the STN as a result of the electrodes. 4. Although unilateral subthalamotomy improves some aspects of parkinsonism, it causes postural abnormalities in animal models of Parkinson's disease. Because bilateral high-frequency STN stimulation improves disease symptoms, is reversible and is not reported to induce postural side-effects, it may be a better surgical therapy for Parkinson's disease than lesioning the STN.
摘要
  1. 中枢多巴胺的缺失是帕金森病的特征,这导致了主要的药物治疗策略,即左旋多巴,一种多巴胺替代疗法。治疗几年后,大多数患者会出现剂量限制性副作用和症状控制丧失。人们对治疗帕金森病的神经外科手术重新产生了兴趣,特别是针对丘脑底核(STN)的新技术,丘脑底核在帕金森病中过度活跃并导致症状发展。2. 我们对实验性诱导帕金森病(使用毒素6-羟基多巴胺诱导)的狨猴和大鼠进行了单侧丘脑底核切开术(通过毒素N-甲基-D-天冬氨酸损伤丘脑底核)。在每种手术前后评估了一系列啮齿动物和灵长类动物共有的相似行为。尸检组织学用于确认损伤。我们还提供了一名帕金森病患者的详细情况,该患者接受了双侧丘脑底核高频刺激,我们对其进行了死后丘脑底核分析。3. 单侧丘脑底核切开术改善了帕金森病灵长类动物的运动不能。然而,猴子和啮齿动物都出现了姿势异常。接受双侧高频刺激的患者运动不能和其他疾病症状有所改善,且没有姿势异常。尸检分析未显示电极导致丘脑底核有实质性损伤。4. 虽然单侧丘脑底核切开术改善了帕金森病的某些方面,但它在帕金森病动物模型中会导致姿势异常。由于双侧丘脑底核高频刺激改善了疾病症状,是可逆的且未报告会诱发姿势副作用,因此它可能是一种比损伤丘脑底核更好的帕金森病手术治疗方法。

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