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首页> 外文期刊>Human Molecular Genetics >Lack of pur-alpha alters postnatal brain development and causes megalencephaly
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Lack of pur-alpha alters postnatal brain development and causes megalencephaly

机译:缺乏pur-alpha会改变出生后的大脑发育并导致巨脑畸形

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Pur-alpha (Purα) plays an important role in a variety of cellular processes including transcriptional regulation, cell proliferation and oncogenic transformation. To better understand the role of Purα in the developing and mature brain, we generated Purα-deficient mice, which we were able to raise to the age of six months. Purα -/- mice were born with no obvious pathological condition. We obtained convincing evidence that lack of Purα prolongs the postnatal proliferation of neuronal precursor cells both in the hippocampus and in the cerebellum, however, without affecting the overall number of postmitotic neurons. Independent of these findings, we observed alterations in the expression and distribution of the dendritic protein MAP2, the translation of which has been proposed previously to be Purα-dependent. At the age of 2 weeks, Purα -/- mice generated a continuous tremor which persisted throughout lifetime. Finally, adult Purα -/- mice displayed a megalencephaly and histopathological findings including axonal swellings and hyperphosphorylation of neurofilaments. Our studies underline the importance of Purα in the proliferation of neuronal precursor cells during postnatal brain development and suggest a role for Pura in the regulation of the expression and cellular distribution of dendritic and axonal proteins. Since recent studies implicate a link between Purα and the fragile X tremor/ataxia syndrome, our Purα -/- mouse model will provide new opportunities for understanding the mechanisms of neurodegeneration.
机译:Pur-alpha(Purα)在多种细胞过程中发挥重要作用,包括转录调控,细胞增殖和致癌转化。为了更好地了解Purα在发育中和成熟的大脑中的作用,我们生成了Purα缺陷型小鼠,能够将其提高到六个月大。 Purα-/-小鼠出生时没有明显的病理状况。我们获得了令人信服的证据,Purα的缺乏会延长海马和小脑中神经元前体细胞的出生后增殖,但是却不影响有丝分裂后神经元的总数。独立于这些发现,我们观察到树突蛋白MAP2的表达和分布发生了变化,以前已经提出其翻译是依赖于Purα的。在2周龄时,Purα-/-小鼠产生了持续的震颤,并持续了一生。最后,成年的Purα-/-小鼠表现出巨头畸形和组织病理学发现,包括轴突肿胀和神经丝过度磷酸化。我们的研究强调了Purα在出生后大脑发育过程中神经元前体细胞增殖中的重要性,并暗示了Pura在调节树突状和轴突蛋白的表达和细胞分布中的作用。由于最近的研究暗示了Purα与脆性X震颤/共济失调综合征之间的联系,因此我们的Purα-/-小鼠模型将为理解神经变性的机制提供新的机会。

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