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首页> 外文期刊>Development >The Abelson tyrosine kinase, the Trio GEF and Enabled interact with the Netrin receptor Frazzled in Drosophila.
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The Abelson tyrosine kinase, the Trio GEF and Enabled interact with the Netrin receptor Frazzled in Drosophila.

机译:Abelson酪氨酸激酶,Trio GEF和Enabled与果蝇中的Netrin受体相互作用。

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摘要

The attractive Netrin receptor Frazzled (Fra), and the signaling molecules Abelson tyrosine kinase (Abl), the guanine nucleotide-exchange factor Trio, and the Abl substrate Enabled (Ena), all regulate axon pathfinding at the Drosophila embryonic CNS midline. We detect genetic and/or physical interactions between Fra and these effector molecules that suggest that they act in concert to guide axons across the midline. Mutations in Abl and trio dominantly enhance fra and Netrin mutant CNS phenotypes, and fra;Abl and fra;trio double mutants display a dramatic loss of axons in a majority of commissures. Conversely, heterozygosity for ena reduces the severity of the CNS phenotype in fra, Netrin and trio,Abl mutants. Consistent with an in vivo role for these molecules as effectors of Fra signaling, heterozygosity for Abl, trio or ena reduces the number of axons that inappropriately cross the midline in embryos expressing the chimeric Robo-Fra receptor. Fra interacts physically with Abl and Trio in GST-pulldown assays and in co-immunoprecipitation experiments. In addition, tyrosine phosphorylation of Trio and Fra is elevated in S2 cells when Abl levels are increased. Together, these data suggest that Abl, Trio, Ena and Fra are integrated into a complex signaling network that regulates axon guidance at the CNS midline.
机译:诱人的Netrin受体Frazzled(Fra)和信号分子Abelson酪氨酸激酶(Abl),鸟嘌呤核苷酸交换因子Trio和Abl底物Enabled(Ena)均调节果蝇胚胎CNS中线的轴突寻路。我们检测到Fra和这些效应分子之间的遗传和/或物理相互作用,表明它们协同作用以指导轴突穿过中线。 Abl和trio中的突变主要增强fra和Netrin突变体CNS表型,而fra; Abl和fra; trio双重突变体在大多数连合中显示出显着的轴突损失。相反,ena的杂合性降低了fra,Netrin和trio,Abl突变体中CNS表型的严重性。与这些分子作为Fra信号转导的效应子在体内的作用一致,Abl,trio或ena的杂合性减少了在表达嵌合Robo-Fra受体的胚胎中不适当地越过中线的轴突的数量。在GST下拉测定法和免疫共沉淀实验中,Fra与Abl和Trio发生物理相互作用。另外,当Abl水平升高时,S2细胞中Trio和Fra的酪氨酸磷酸化升高。总之,这些数据表明,Abl,Trio,Ena和Fra已整合到一个复杂的信号网络中,该网络调节CNS中线的轴突导向。

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