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Rab21 GTPase 对于大脑皮层中的神经元发育和迁移是必需的。

The GTPase Rab21 is required for neuronal development and migration in the cerebral cortex.

机构信息

Departamento de Química Biológica Ranwell Caputto, Facultad de Ciencias Químicas, CIQUIBIC-CONICET-Universidad Nacional de Córdoba, Córdoba, Argentina.

Axonal Growth and Regeneration, German Center for Neurodegenarative Diseases, Bonn, Germany.

出版信息

J Neurochem. 2023 Sep;166(5):790-808. doi: 10.1111/jnc.15925. Epub 2023 Aug 3.

Abstract

Development of the mammalian neocortex requires proper inside-out migration of developing cortical neurons from the germinal ventricular zone toward the cortical plate. The mechanics of this migration requires precise coordination of different cellular phenomena including cytoskeleton dynamics, membrane trafficking, and cell adhesion. The small GTPases play a central role in all these events. The small GTPase Rab21 regulates migration and neurite growth in developing neurons. Moreover, regulators and effectors of Rab21 have been implicated in brain pathologies with cortical malformations, suggesting a key function for the Rab21 signaling pathway in cortical development. Mechanistically, it has been posited that Rab21 influences cell migration by controlling the trafficking of endocytic vesicles containing adhesion molecules. However, direct evidence of the participation of Rab21 or its mechanism of action in the regulation of cortical migration is still incomplete. In this study, we demonstrate that Rab21 plays a critical role in the differentiation and migration of pyramidal neurons by regulating the levels of the amyloid precursor protein on the neuronal cell surface. Rab21 loss of function increased the levels of membrane-exposed APP, resulting in impaired cortical neuronal differentiation and migration. These findings further our understanding of the processes governing the development of the cerebral cortex and shed light onto the molecular mechanisms behind cortical development disorders derived from the malfunctioning of Rab21 signaling effectors.

摘要

哺乳动物大脑皮层的发育需要发育中的皮质神经元从生发室带沿着正确的内外迁移方向朝着皮质板迁移。这种迁移的机制需要精确协调不同的细胞现象,包括细胞骨架动力学、膜运输和细胞黏附。小分子 GTP 酶在所有这些事件中都起着核心作用。小分子 GTP 酶 Rab21 调节发育中的神经元的迁移和突起生长。此外,Rab21 的调节剂和效应物已被牵连到具有皮质畸形的脑病理学中,这表明 Rab21 信号通路在皮质发育中具有关键功能。从机制上讲,有人提出 Rab21 通过控制含有黏附分子的内吞小泡的运输来影响细胞迁移。然而,Rab21 参与调节皮质迁移的直接证据及其作用机制仍然不完整。在这项研究中,我们证明 Rab21 通过调节神经元细胞表面的淀粉样前体蛋白(APP)的水平,在锥体神经元的分化和迁移中发挥关键作用。Rab21 功能丧失会增加暴露在细胞膜上的 APP 水平,从而导致皮质神经元分化和迁移受损。这些发现进一步了解了大脑皮层发育的调控过程,并揭示了源自 Rab21 信号效应器功能障碍的皮质发育障碍的分子机制。

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