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Pak1及其T212磷酸化形式在发育中的啮齿动物的神经元和上皮细胞中积累。

Pak1 and its T212 phosphorylated form accumulate in neurones and epithelial cells of the developing rodent.

作者信息

Zhong Julia L, Banerjee Monisha D, Nikolic Margareta

机构信息

Developmental Neurobiology MRC Centre, King's College London, London, United Kingdom.

出版信息

Dev Dyn. 2003 Sep;228(1):121-7. doi: 10.1002/dvdy.10351.

Abstract

The serine/threonine kinase Pak1 is a target of the RhoGTPases Rac and Cdc42 and an important regulator of cell morphology and migration. Recent work from several laboratories has indicated that Pak1 controls microtubule dynamics as well as the organisation of F-actin microfilaments. Pak1 is phosphorylated on T212 by the p35/Cdk5 or cyclin B1/Cdc2 kinase in postmitotic neurones and mitotic cells, respectively. To understand its function during development, we have carried out a detailed temporal and spatial analysis of Pak1 expression and phosphorylation on T212. In the embryonic forebrain, Pak1 and Pak1T212(PO4) were seen to accumulate in the corpus callosum, intermediate zone, lateral olfactory tracts, and anterior commissures. Epithelial cells of the mouse embryo lung, kidney, intestine, and skin also exhibited high levels of Pak1 and Pak1T212(PO4), suggesting a previously unsuspected role in epithelial differentiation. Pak1T212(PO4) was undetectable in all adult tissues. Together, these data indicate a specific, developmentally regulated role of the Pak1 kinase.

摘要

丝氨酸/苏氨酸激酶Pak1是RhoGTPases Rac和Cdc42的作用靶点,也是细胞形态和迁移的重要调节因子。多个实验室最近的研究表明,Pak1控制微管动力学以及F-肌动蛋白微丝的组织。在有丝分裂后的神经元和有丝分裂细胞中,Pak1分别被p35/Cdk5或细胞周期蛋白B1/Cdc2激酶在T212位点磷酸化。为了解其在发育过程中的功能,我们对Pak1的表达以及T212位点的磷酸化进行了详细的时空分析。在胚胎前脑中,Pak1和磷酸化的Pak1(Pak1T212(PO4))在胼胝体、中间带、外侧嗅束和前连合中积累。小鼠胚胎肺、肾、肠和皮肤的上皮细胞也表现出高水平的Pak1和Pak1T212(PO4),表明其在上皮分化中具有先前未被怀疑的作用。在所有成年组织中均未检测到Pak1T212(PO4)。这些数据共同表明了Pak1激酶具有特定的、受发育调控的作用。

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