ProNGF 通过 p75NTR 诱导 PTEN 抑制脑神经元中 Trk 介导的存活信号。
ProNGF induces PTEN via p75NTR to suppress Trk-mediated survival signaling in brain neurons.
机构信息
Department of Biological Science, Rutgers University, Newark, New Jersey 07102, USA.
出版信息
J Neurosci. 2010 Nov 17;30(46):15608-15. doi: 10.1523/JNEUROSCI.2581-10.2010.
Proneurotrophins and mature neurotrophins activate different signaling pathways with distinct effects on their target cells: proneurotrophins can induce apoptotic signaling via p75(NTR), whereas mature neurotrophins activate Trk receptors to influence survival and differentiation. Here, we demonstrate that the PTEN (phosphatase and tensin homolog deleted on chromosome 10) phosphatase represents a novel switch between the survival and apoptotic signaling pathways in rat CNS neurons. Simultaneous activation of p75(NTR) by proNGF and TrkB signaling by BDNF elicited apoptosis despite TrkB phosphorylation. Apoptosis induced by p75(NTR) required suppression of TrkB-induced phosphoinositide-3 kinase signaling, mediated by induction of PTEN, for apoptosis to proceed. Inhibition of PTEN restored the ability of BDNF to phosphorylate Akt and protect cultured basal forebrain neurons from proNGF-induced death. In vivo, inhibition or knockdown of PTEN after pilocarpine-induced seizures protected CNS neurons from p75(NTR)-mediated death, demonstrating that PTEN is a crucial factor mediating the balance between p75(NTR)-induced apoptotic signaling and Trk-mediated survival signaling in brain neurons.
原神经营养因子和成熟神经营养因子通过不同的信号通路激活,对其靶细胞产生不同的影响:原神经营养因子可以通过 p75(NTR)诱导凋亡信号,而成熟神经营养因子则激活 Trk 受体来影响存活和分化。在这里,我们证明了 PTEN(第 10 号染色体缺失的磷酸酶和张力蛋白同源物)磷酸酶是大鼠中枢神经系统神经元中存活和凋亡信号通路之间的一个新的开关。尽管 BDNF 激活了 TrkB,但同时激活 p75(NTR)的 proNGF 和 TrkB 信号会引发细胞凋亡。p75(NTR)诱导的凋亡需要抑制 TrkB 诱导的磷酯酰肌醇-3 激酶信号,这是通过诱导 PTEN 介导的,凋亡才能进行。PTEN 的抑制恢复了 BDNF 磷酸化 Akt 的能力,并保护培养的基底前脑神经元免受 proNGF 诱导的死亡。在体内,匹鲁卡品诱导癫痫发作后抑制或敲低 PTEN 可保护中枢神经系统神经元免受 p75(NTR)介导的死亡,表明 PTEN 是介导大脑神经元中 p75(NTR)诱导的凋亡信号和 Trk 介导的存活信号之间平衡的关键因素。
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