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首页> 外文期刊>The Journal of biological chemistry >Trio Is a Key Guanine Nucleotide Exchange Factor Coordinating Regulation of the Migration and Morphogenesis of Granule Cells in the Developing Cerebellum
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Trio Is a Key Guanine Nucleotide Exchange Factor Coordinating Regulation of the Migration and Morphogenesis of Granule Cells in the Developing Cerebellum

机译:三重奏是一种关键的鸟嘌呤核苷酸交换因子协调调节颗粒细胞中颗粒细胞的迁移和形态发生

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摘要

Orchestrated regulation of neuronal migration and morphogenesis is critical for neuronal development and establishment of functional circuits, but its regulatory mechanism is incompletely defined. We established and analyzed mice with neural-specific knock-out of Trio, a guanine nucleotide exchange factor with multiple guanine nucleotide exchange factor domains. Knock-out mice showed defective cerebella and severe signs of ataxia. Mutant cerebella had no granule cells in the internal granule cell layer due to aberrant granule cell migration as well as abnormal neurite growth. Trio-deficient granule cells showed reduced extension of neurites and highly branched and misguided processes with perturbed stabilization of actin and microtubules. Trio deletion caused down-regulation of the activation of Rac1, RhoA, and Cdc42, and mutant granule cells appeared to be unresponsive to neurite growth-promoting molecules such as Netrin-1 and Semaphorin 6A. These results suggest that Trio may be a key signal module for the orchestrated regulation of neuronal migration and morphogenesis during cerebellar development. Trio may serve as a signal integrator decoding extrinsic signals to Rho GTPases for cytoskeleton organization.
机译:策划的神经元迁移和形态发生的调节对于神经元开发和功能性电路的建立至关重要,但其调节机制是不完全定义的。我们建立并分析了具有神经特异性敲除TRIO的小鼠,具有多种鸟嘌呤核苷酸交换系数域的鸟嘌呤核苷酸交换因子。敲除小鼠显示出缺陷的脑脑和共济失调的严重迹象。由于异常的颗粒细胞迁移以及神经突生长异常,突变体内脑细胞中没有颗粒细胞。三重量缺乏颗粒细胞显示神经菌素和高度分枝和误导过程的延伸减少,具有肌动蛋白和微管的扰动稳定。三重血缺失导致Rac1,RhoA和CDC42的激活的下调,突变颗粒细胞似乎对神经突生长促进分子如Netrin-1和信号蛋白6a无响应。这些结果表明,三重组可以是用于在小脑发育过程中衡心神经元迁移和形态发生的核心调节的关键信号模块。 TRIO可以用作信号积分器解码外在信号,用于细胞骨架组织的RHO GTH酶。

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