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Neuropathology of primary adult-onset dystonia.

机译:神经病理学的主要成人肌张力障碍。

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BACKGROUND: Idiopathic adult-onset primary dystonia usually affects the upper body and remains focal. Underlying mechanisms are unknown, and there are only limited neuropathologic studies in the literature. Recently, ubiquitinated perinuclear inclusion bodies were found in the brainstem of patients with DYT1-related dystonia. In X-linked recessive dystonia-parkinsonism, neuronal loss in the striosome compartment of the striatum has been described. However, it was unclear whether these changes are characteristic of these particular disorders or an epiphenomenon of dystonic conditions in general. METHODS: Six cases of adult-onset dystonia and four controls were studied using immunohistochemistry to determine the presence of inclusion bodies immunoreactive for torsinA, ubiquitin, and laminA/C in the brainstem. The distribution of calcineurin expressing neurons in the striatum was also determined to ascertain whether there is loss of neurons in the striosome compartment. RESULTS: In contrast to early-onsetdystonia, neuronal inclusions immunoreactive for torsinA, ubiquitin, and laminA/C were not present in the brainstem nuclei. There was no apparent loss of the striatal striosome compartment. CONCLUSION: Our findings suggest that the underlying mechanism in the adult-onset primary torsion dystonia is different from that of early-onset DYT1-related dystonia and also DYT3 X-linked recessive dystonia-parkinsonism. Alternative mechanisms may underpin the pathophysiology of adult-onset primary dystonia.
机译:背景:特发性成人初选肌张力障碍通常影响上半身和仍然是焦点。还有neuropathologic有限研究在文献中。ubiquitinated细胞核周围的包涵体患者的脑干中找到DYT1-related肌张力障碍。dystonia-parkinsonism,神经元的损失striosome隔间的纹状体描述。这些特殊的变化特征疾病或矛盾的的附带现象条件一般。成人肌张力障碍和四个控制使用免疫组织化学研究来确定包涵体的存在免疫反应性的torsinA、泛素和板/ C脑干。表达在纹状体神经元也决心查明是否有损失神经元striosome隔间。early-onsetdystonia相比,神经元夹杂物对torsinA免疫反应性的,泛素,和板/ C没有出现在脑干细胞核。纹状体striosome隔间。研究结果表明,底层机制成人主要扭转肌张力障碍不同于早发型DYT1-related肌张力障碍也DYT3 x连锁隐性dystonia-parkinsonism。支撑的病理生理学成人原发性肌张力障碍。

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