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首页> 外文期刊>Neuroscience: An International Journal under the Editorial Direction of IBRO >Neuronal production and precursor proliferation defects in the neocortex of mice with loss of function in the canonical Wnt signaling pathway.
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Neuronal production and precursor proliferation defects in the neocortex of mice with loss of function in the canonical Wnt signaling pathway.

机译:小鼠新皮层中神经元的产生和前体增殖缺陷,以及经典Wnt信号通路功能丧失。

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摘要

To better understand the function of the Wnt pathway in the developing telencephalon, we analyzed neocortical development in low density lipoprotein receptor-related protein (LRP) 6 mutants. LRP6 mutant mice are hypomorphic for the canonical Wnt signaling pathway and have hypoplasia of the developing neocortex. While early telencephalic morphogenesis is largely intact in these mice, probably due to compensation by LRP5, the mutant mice develop a dramatically thinner cortical plate. There is a prominent reduction of neurogenesis leading to a thin cortical plate. Reduced proliferation late in gestation probably also contributes to the hypoplasia. Although there are marked decreases in the numbers of layer 6 and layers 2-4 neurons all laminar identities are generated and there is no evidence of compensatory increases in layer 5 neurons. In addition, LRP6 mutants have partial penetrance of a complex of cortical dysmorphologies resembling those found in patients with developmental forms of epilepsy and mental retardation. These include ventricular and marginal zone heterotopias and cobblestone lissencephaly. This analysis demonstrates that canonical Wnt signaling is required for a diverse array of developmental processes in the neocortex in addition to the previously known roles in regulating precursor proliferation and patterning.
机译:为了更好地了解Wnt通路在正在​​发展的端脑中的功能,我们分析了低密度脂蛋白受体相关蛋白(LRP)6突变体中的新皮质发育。 LRP6突变小鼠的经典Wnt信号通路是亚型的,并且发育中的新皮层发育不全。尽管这些小鼠的早期远脑形态发生在很大程度上是完整的,这可能是由于LRP5的补偿所致,但突变小鼠的皮质板却显着变薄。神经发生显着减少,导致皮质板薄。妊娠后期增殖减少可能也导致发育不全。尽管第6层和第2-4层神经元的数量显着减少,但所有层状身份均会生成,并且没有证据表明第5层神经元的补偿性增加。此外,LRP6突变体具有部分皮质畸形的外显率,类似于在患有癫痫和智力低下的发育形式的患者中发现的那些。这些包括心室和边缘区异位症和鹅卵石性脑病。该分析表明,除了先前已知的调节前体增殖和构型的作用外,新皮质中多种发育过程还需要规范的Wnt信号传导。

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