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首页> 外文期刊>Frontiers in Cellular Neuroscience >Transient Developmental Purkinje Cell Axonal Torpedoes in Healthy and Ataxic Mouse Cerebellum
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Transient Developmental Purkinje Cell Axonal Torpedoes in Healthy and Ataxic Mouse Cerebellum

机译:健康和自律性小鼠小脑的瞬态发育浦肯野细胞轴突鱼雷。

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Information is carried out of the cerebellar cortical microcircuit via action potentials propagated along Purkinje cell axons. In several human neurodegenerative diseases, focal axonal swellings on Purkinje cells – known as torpedoes – have been associated with Purkinje cell loss. Interestingly, torpedoes are also reported to appear transiently during development in rat cerebellum. The function of Purkinje cell axonal torpedoes in health as well as in disease is poorly understood. We investigated the properties of developmental torpedoes in the postnatal mouse cerebellum of wild-type and transgenic mice. We found that Purkinje cell axonal torpedoes transiently appeared on axons of Purkinje neurons, with the largest number of torpedoes observed at postnatal day 11 (P11). This was after peak developmental apoptosis had occurred, when Purkinje cell counts in a lobule were static, suggesting that most developmental torpedoes appear on axons of neurons that persist into adulthood. We found that developmental torpedoes were not associated with a presynaptic GABAergic marker, indicating that they are not synapses. They were seldom found at axonal collateral branch points, and lacked microglia enrichment, suggesting that they are unlikely to be involved in axonal refinement. Interestingly, we found several differences between developmental torpedoes and disease-related torpedoes: developmental torpedoes occurred largely on myelinated axons, and were not associated with changes in basket cell innervation on their parent soma. Disease-related torpedoes are typically reported to contain neurofilament; while the majority of developmental torpedoes did as well, a fraction of smaller developmental torpedoes did not. These differences indicate that developmental torpedoes may not be functionally identical to disease-related torpedoes. To study this further, we used a mouse model of spinocerebellar ataxia type 6 (SCA6), and found elevated disease-related torpedo number at 2 years. However, we found normal levels of developmental torpedoes in these mice. Our findings suggest that the transient emergence of Purkinje cell axonal torpedoes during the second postnatal week in mice represents a normal morphological feature in the developing cerebellar microcircuit.
机译:信息是通过沿Purkinje细胞轴突传播的动作电位从小脑皮质微电路中获得的。在几种人类神经退行性疾病中,浦肯野细胞上的局灶性轴突肿胀(称为鱼雷)与浦肯野细胞的丢失有关。有趣的是,据报道,鱼雷在大鼠小脑发育过程中会短暂出现。人们对浦肯野细胞轴突鱼雷在健康和疾病中的功能了解甚少。我们调查了野生型和转基因小鼠产后小鼠小脑中发育鱼雷的特性。我们发现浦肯野细胞轴突鱼雷瞬时出现在浦肯野神经元的轴突上,在出生后第11天(P11)观察到最多的鱼雷。这是在发生峰值发育凋亡之后,小叶中的浦肯野细胞计数是静态的,这表明大多数发育鱼雷出现在持续到成年的神经元轴突上。我们发现发育鱼雷与突触前的GABAergic标记无关,表明它们不是突触。很少在轴突侧支分支处发现它们,并且缺乏小胶质细胞富集,这表明它们不太可能参与轴突的提纯。有趣的是,我们发现发育型鱼雷与疾病相关的鱼雷之间存在一些差异:发育型鱼雷主要发生在有髓的轴突上,并且与它们的父体的篮状细胞神经支配的变化无关。据报道,与疾病有关的鱼雷含有神经丝。虽然大多数发育鱼雷也能做到,但一小部分发育鱼雷却没有。这些差异表明,发育中的鱼雷可能与疾病相关的鱼雷在功能上并不相同。为了进一步研究,我们使用了6型脊髓小脑共济失调的小鼠模型(SCA6),并发现2年时与疾病相关的鱼雷数量增加。但是,我们在这些小鼠中发现了正常的鱼雷发育水平。我们的研究结果表明,小鼠出生后第二周浦肯野细胞轴突鱼雷的短暂出现代表小脑微电路发育中的正常形态特征。

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