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Rho、Rac和Cdc42对树突生长和重塑的调控

Regulation of dendritic growth and remodeling by Rho, Rac, and Cdc42.

作者信息

Threadgill R, Bobb K, Ghosh A

机构信息

Department of Neuroscience, Johns Hopkins University School of Medicine, Baltimore, Maryland 21205, USA.

出版信息

Neuron. 1997 Sep;19(3):625-34. doi: 10.1016/s0896-6273(00)80376-1.

Abstract

The acquisition of cell type-specific morphologies is a central feature of neuronal differentiation and has important consequences for nervous system function. To begin to identify the underlying molecular mechanisms, we have explored the role of Rho-related GTPases in the dendritic development of cortical neurons. Expression of dominant negative mutants of Rac or Cdc42, the Rho-inhibitory molecule C3 transferase, or the GTPase-activating protein RhoGAP p190 causes a marked reduction in the number of primary dendrites in nonpyramidal (multipolar) neurons and in the number of basal dendrites in neurons with pyramidal morphologies. Conversely, the expression of constitutively active mutants of Rho, Rac, or Cdc42 leads to an increase in the number of primary and basal dendrites. In cortical cultures, as in vivo, dendritic remodeling leads to an apparent transformation from pyramidal to nonpyramidal morphologies over time. Strikingly, this shift in favor of nonpyramidal morphologies is also inhibited by the expression of dominant negative mutants of Cdc42 and Rac and by RhoGAP p190. These observations indicate that Rho, Rac, and Cdc42 play a central role in dendritic development and suggest that differential activation of Rho-related GTPases may contribute to the generation of morphological diversity in the developing cortex.

摘要

获得细胞类型特异性形态是神经元分化的核心特征,对神经系统功能具有重要影响。为了开始确定其潜在的分子机制,我们探讨了Rho相关GTP酶在皮质神经元树突发育中的作用。Rac或Cdc42的显性负性突变体、Rho抑制分子C3转移酶或GTP酶激活蛋白RhoGAP p190的表达,会导致非锥体(多极)神经元的初级树突数量以及具有锥体形态的神经元的基底树突数量显著减少。相反,Rho、Rac或Cdc42的组成型活性突变体的表达会导致初级和基底树突数量增加。在皮质培养物中,与在体内一样,随着时间的推移,树突重塑会导致从锥体形态到非锥体形态的明显转变。引人注目的是,Cdc42和Rac的显性负性突变体以及RhoGAP p190的表达也会抑制这种向非锥体形态的转变。这些观察结果表明,Rho、Rac和Cdc42在树突发育中起核心作用,并表明Rho相关GTP酶的差异激活可能有助于发育中的皮质中形态多样性的产生。

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