Heise Claire E, Teo Zui Chih, Wallace Bradley A, Ashkan Keyoumars, Benabid Alim-Louis, Mitrofanis John
Department of Anatomy & Histology, University of Sydney, Australia.
Anat Embryol (Berl). 2005 Nov;210(4):287-302. doi: 10.1007/s00429-005-0053-1. Epub 2005 Nov 12.
We explore the patterns of cell loss in the pedunculopontine tegmental nucleus (PpT), a major locomotor and muscle tone suppression centre of the brainstem, in two animal models of Parkinson disease, namely MPTP (methyl-4-phenyl-1,2,3,6-tetrahydropyridine)-treated monkeys and 6-hydroxydopamine(6OHDA)-lesioned rats. Although there have been many studies documenting the loss of dopaminergic cells from the substantia nigra in these animal models, there has been little, if any, documentation of a loss of cells in the PpT. Results were obtained from macaque monkeys (Macaca fascicularis) and Sprague-Dawley rats. For the monkey series, animals were injected intramuscularly with MPTP (0.2 mg/kg) for 8 days consecutively and then allowed to survive for 21 days thereafter. Each monkey underwent behavioural assessment for parkinsonian symptoms. For the rat series, 6OHDA was injected into the midbrain using stereotactic coordinates. Rats were then allowed to survive for either 7, 14, 28, or 84 days thereafter. Monkey and rat brains were aldehyde-fixed and processed for routine tyrosine hydroxylase (TH; to label nigral dopaminergic cells) and nitric oxide synthase (NOs; to label PpT cholinergic cells) immunocytochemistry. In monkeys, the morphology, distribution and number of NOs(+) cells in the controls and MPTP-treated cases were very similar. In fact, in terms of number, there was only a 1% difference in the mean cell number between the controls and MPTP-treated cases. A comparable pattern was evident in 6OHDA-lesioned rats; there was no substantial difference in morphology, distribution and number of NOs(+) cells on the 6OHDA-lesioned cases when compared to the controls at each of the survival periods post-surgery. In summary, we show no loss of the large cholinergic/NOs(+) cells in the PpT in two animal models of Parkinson disease. This is in contrast to the heavy loss of these cells reported by previous findings in idiopathic Parkinson disease in patients.
我们在两种帕金森病动物模型中,即1-甲基-4-苯基-1,2,3,6-四氢吡啶(MPTP)处理的猴子和6-羟基多巴胺(6OHDA)损伤的大鼠中,研究了脑桥脚被盖核(PpT)的细胞丢失模式。PpT是脑干中主要的运动和肌张力抑制中心。尽管已有许多研究记录了这些动物模型中黑质多巴胺能细胞的丢失,但关于PpT中细胞丢失的记录却很少,即便有也寥寥无几。研究结果来自猕猴(食蟹猴)和Sprague-Dawley大鼠。对于猴子系列,动物连续8天肌肉注射MPTP(0.2mg/kg),然后让其存活21天。每只猴子都接受了帕金森病症状的行为评估。对于大鼠系列,使用立体定位坐标将6OHDA注入中脑。然后让大鼠分别存活7、14、28或84天。猴子和大鼠的大脑用醛固定,并进行常规酪氨酸羟化酶(TH;标记黑质多巴胺能细胞)和一氧化氮合酶(NOs;标记PpT胆碱能细胞)免疫细胞化学处理。在猴子中,对照组和MPTP处理组中NOs(+)细胞的形态、分布和数量非常相似。事实上,就数量而言,对照组和MPTP处理组之间的平均细胞数仅相差1%。在6OHDA损伤的大鼠中也出现了类似的模式;与术后每个存活期的对照组相比,6OHDA损伤组中NOs(+)细胞的形态、分布和数量没有实质性差异。总之,我们发现在两种帕金森病动物模型中,PpT中大型胆碱能/NOs(+)细胞没有丢失。这与先前在特发性帕金森病患者中报道的这些细胞的大量丢失形成对比。
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