TrkB-Shc位点通过MEK和P13激酶发出神经元存活和局部轴突生长的信号。
The TrkB-Shc site signals neuronal survival and local axon growth via MEK and P13-kinase.
作者信息
Atwal J K, Massie B, Miller F D, Kaplan D R
机构信息
Center for Neuronal Survival, McGill University, Montreal, Quebec, Canada.
出版信息
Neuron. 2000 Aug;27(2):265-77. doi: 10.1016/s0896-6273(00)00035-0.
To determine how signals emanating from Trk transmit neurotrophin actions in primary neurons, we tested the ability of TrkB mutated at defined effector binding sites to promote sympathetic neuron survival or local axon growth. TrkB stimulated signaling proteins and induced survival and growth in a manner similar to TrkA. TrkB mutated at the Shc binding site supported survival and growth poorly relative to wild-type TrkB, whereas TrkB mutated at the PLC-gamma1 binding site supported growth and survival well. TrkB-mediated neuronal survival was dependent on P13-kinase and to a lesser extent MEK activity, while growth depended upon both MEK and P13-kinase activities. These results indicate that the TrkB-Shc site mediates both neuronal survival and axonal outgrowth by activating the P13-kinase and MEK signaling pathways.
为了确定源自Trk的信号如何在初级神经元中传递神经营养因子的作用,我们测试了在特定效应器结合位点发生突变的TrkB促进交感神经元存活或局部轴突生长的能力。TrkB刺激信号蛋白并以类似于TrkA的方式诱导存活和生长。相对于野生型TrkB,在Shc结合位点发生突变的TrkB对存活和生长的支持较差,而在PLC-γ1结合位点发生突变的TrkB对生长和存活的支持良好。TrkB介导的神经元存活依赖于PI3激酶,在较小程度上依赖于MEK活性,而生长则依赖于MEK和PI3激酶的活性。这些结果表明,TrkB-Shc位点通过激活PI3激酶和MEK信号通路介导神经元存活和轴突生长。
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