首页> 美国卫生研究院文献>The Journal of Biophysical and Biochemical Cytology >Essential role of B-Raf in oligodendrocyte maturation and myelination during postnatal central nervous system development
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Essential role of B-Raf in oligodendrocyte maturation and myelination during postnatal central nervous system development

机译:B-Raf在产后中枢神经系统发育过程中在少突胶质细胞成熟和髓鞘形成中的重要作用

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摘要

Mutations in the extracellular signal-regulated kinase (ERK) pathway, particularly in the mitogen-activated protein kinase/ERK kinase (MEK) activator B-Raf, are associated with human tumorigenesis and genetic disorders. Hence, B-Raf is a prime target for molecule-based therapies, and understanding its essential biological functions is crucial for their success. B-Raf is expressed preferentially in cells of neuronal origin. Here, we show that in mice, conditional ablation of B-Raf in neuronal precursors leads to severe dysmyelination, defective oligodendrocyte differentiation, and reduced ERK activation in brain. Both B-Raf ablation and chemical inhibition of MEK impair oligodendrocyte differentiation in vitro. In glial cell cultures, we find B-Raf in a complex with MEK, Raf-1, and kinase suppressor of Ras. In B-Raf–deficient cells, more Raf-1 is recruited to MEK, yet MEK/ERK phosphorylation is impaired. These data define B-Raf as the rate-limiting MEK/ERK activator in oligodendrocyte differentiation and myelination and have implications for the design and use of Raf inhibitors.
机译:细胞外信号调节激酶(ERK)途径中的突变,特别是促分裂原活化的蛋白激酶/ ERK激酶(MEK)激活剂B-Raf中的突变,与人类肿瘤发生和遗传疾病有关。因此,B-Raf是基于分子疗法的主要靶标,而了解其基本生物学功能对其成功至关重要。 B-Raf优先在神经元起源的细胞中表达。在这里,我们显示在小鼠中,神经元前体中B-Raf的条件性消融会导致严重的髓鞘异常,少突胶质细胞分化以及脑内ERK激活降低。 B-Raf消融和MEK的化学抑制均会损害少突胶质细胞的体外分化。在神经胶质细胞培养物中,我们发现B-Raf与MEK,Raf-1和Ras激酶抑制剂复合。在缺乏B-Raf的细胞中,更多Raf-1被募集到MEK,但MEK / ERK磷酸化受到损害。这些数据将B-Raf定义为少突胶质细胞分化和髓鞘形成的限速MEK / ERK活化剂,并且对Raf抑制剂的设计和使用具有影响。

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