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在摇晃突变型大鼠中,小脑浦肯野细胞通过凋亡死亡。

Cerebellar Purkinje cells die by apoptosis in the shaker mutant rat.

作者信息

Erekat Nour S

机构信息

Department of Anatomy, Faculty of Medicine, Jordan University of Science and Technology (JUST), Jordan.

出版信息

Brain Res. 2017 Feb 15;1657:323-332. doi: 10.1016/j.brainres.2016.12.025. Epub 2016 Dec 28.

DOI:10.1016/j.brainres.2016.12.025
PMID:28040459
Abstract

Cerebellar Purkinje cells (PCs) die in humans leading to a variety of diseases including ataxia and essential tremor. The etiology underlying PC death is poorly understood. Shaker mutant rat is a unique animal model of progressive PC degeneration that is compartmentalized and of adult-onset. In shaker mutant rats, hereditary degeneration of at risk PCs occurs between 7 and 14 postnatal weeks of age as a natural phenotypic expression of the shaker mutation and at earlier or later ages depending upon experimental conditions in restricted anterior (ADC) and posterior (PDC) vermal degeneration compartments. Secure PCs in a flocculonodular survival compartment (FNSC) always survive. In this study, we investigated DNA fragmentation and active caspase-3 expression characteristic of apoptosis using immunofluorescence and fluorescence microscopy. We also sought to confirm the occurrence of apoptosis in at risk PCs using transmission electron microscope. Purkinje neurons were the only cerebellar cells labeled for TUNEL and immunoreactive to active caspase-3 in the shaker mutant. Active caspase-3 expression observed was spatially and temporally congruous with the pattern of calbindin immunolabeling of degenerating PCs that is characterized by dendritic atrophy, shrinkage of PC cell bodies and the appearance of PC axonal torpedoes. DNA fragmentation, detected by TUNEL, as well as ultrastructural morphological changes characteristic for apoptosis, provided additional evidence for the occurrence of apoptosis in at risk PCs.

摘要

小脑浦肯野细胞(PCs)在人类中死亡会导致包括共济失调和特发性震颤在内的多种疾病。PCs死亡的病因尚不清楚。震颤突变大鼠是进行性PCs变性的独特动物模型,这种变性具有分区性且为成年发病。在震颤突变大鼠中,处于危险中的PCs的遗传性变性在出生后7至14周龄之间发生,这是震颤突变的自然表型表达,并且根据受限的前(ADC)和后(PDC)蚓部变性区室中的实验条件,在更早或更晚的年龄发生。在绒球小结叶存活区室(FNSC)中安全的PCs总是存活下来。在本研究中,我们使用免疫荧光和荧光显微镜研究了凋亡特有的DNA片段化和活性半胱天冬酶-3表达特征。我们还试图使用透射电子显微镜确认处于危险中的PCs中凋亡的发生。在震颤突变体中,浦肯野神经元是唯一被TUNEL标记且对活性半胱天冬酶-3有免疫反应的小脑细胞。观察到的活性半胱天冬酶-3表达在空间和时间上与退化PCs的钙结合蛋白免疫标记模式一致,其特征为树突萎缩、PCs细胞体缩小以及PCs轴突鱼雷的出现。通过TUNEL检测到的DNA片段化以及凋亡特有的超微结构形态变化,为处于危险中的PCs中凋亡的发生提供了额外证据。

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