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LRRK2: an éminence grise of Wnt-mediated neurogenesis?

机译:LRRK2:Wnt介导的神经发生的显著性?

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摘要

The importance of leucine-rich repeat kinase 2 (LRRK2) to mature neurons is well-established, since mutations in PARK8, the gene encoding LRRK2, are the most common known cause of Parkinson’s disease. Nonetheless, despite the LRRK2 knockout mouse having no overt neurodevelopmental defect, numerous lines of in vitro data point toward a central role for this protein in neurogenesis. Roles for LRRK2 have been described in many key processes, including neurite outgrowth and the regulation of microtubule dynamics. Moreover, LRRK2 has been implicated in cell cycle control, suggesting additional roles in neurogenesis that precede terminal differentiation. However, we contend that the suggested function of LRRK2 as a scaffolding protein at the heart of numerous Wnt signaling cascades provides the most tantalizing link to neurogenesis in the developing brain. Numerous lines of evidence show a critical requirement for multiple Wnt pathways in the development of certain brain regions, not least the dopaminergic neurons of the ventral mid-brain. In conclusion, these observations indicate a function of LRRK2 as a subtle yet critical mediator of the action of Wnt ligands on developing neurons. We suggest that LRRK2 loss- or gain-of-function are likely modifiers of developmental phenotypes seen in animal models of Wnt signaling deregulation, a hypothesis that can be tested by cross-breeding relevant genetically modified experimental strains.
机译:富含亮氨酸的重复激酶2(LRRK2)对成熟神经元的重要性已得到公认,因为编码LRRK2的基因PARK8的突变是帕金森氏病最常见的病因。尽管如此,尽管LRRK2基因敲除小鼠没有明显的神经发育缺陷,但许多体外数据表明该蛋白在神经发生中起着重要作用。 LRRK2的作用已在许多关键过程中进行了描述,包括神经突生长和微管动力学调节。而且,LRRK2与细胞周期控制有关,提示在终末分化之前的神经发生中还有其他作用。但是,我们认为,LRRK2作为支架蛋白的功能在众多Wnt信号级联反应的心脏处提供,对发育中的神经发生提供了最诱人的联系。许多证据表明,在某些大脑区域,尤其是腹中脑的多巴胺能神经元的发育中,需要多种Wnt途径。总之,这些观察结果表明LRRK2作为Wnt配体对发育中的神经元的作用的微妙而关键的介体。我们建议LRRK2功能丧失或获得功能可能是在Wnt信号去调控的动物模型中看到的发育表型的修饰物,该假说可以通过杂交相关的基因修饰实验株来检验。

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