B-RAF drives regenerative axon growth in the optic nerve in vivo

B-RAF 驱动体内视神经再生轴突生长

• 批准号: 8520804
• 负责人: Jian Zhong
• 金额: $ 20.47万
• 依托单位: WINIFRED MASTERSON BURKE MED RES INST
• 依托单位国家: 美国
• 财政年份: 2012
• 资助国家: 美国
• 起止时间: 2012-05-01 至 2017-04-30
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/8520804
• 关键词: 1-Phosphatidylinositol 3-Kinase; Address; Adult; Afferent Neurons; Alleles; Axon; Biological Assay; Cell Nucleus; Cells; Collaborations; Data; Degenerative Disorder; Development; Drug Delivery Systems; Embryo; Failure; Future; Genetic Recombination; Glaucoma; Goals; Growth; Image; Injury; Institutes; Knock-out; MAP Kinase Modules; MAP2K1 gene; MAPK1 gene; MAPK3 gene; MEKs; Mediating; Mediator of activation protein; Mitogen-Activated Protein Kinases; Modeling; Mus; Natural regeneration; Nerve Crush; Nervous System Trauma; Neuraxis; Neurites; Neurons; Optic Nerve; Optic Nerve Injuries; Optic tract structure; PTEN gene; Pathway interactions; Patients; Pharmaceutical Preparations; Phosphotransferases; Photons; Procedures; Proteins; Proto-Oncogene Proteins c-akt; Public Health; Recovery; Recovery of Function; Rehabilitation therapy; Retina; Retinal Ganglion Cells; Role; Sensory; Serum Response Factor; Signal Pathway; Signal Transduction; Signal Transduction Pathway; Signaling Molecule; Tamoxifen; Testing; Time; Translational Research; Trauma; Vision; axon growth; axon regeneration; base; central nervous system injury; disability; gain of function; improved; in vivo; injured; loss of function; mouse model; neurotrophic factor; novel; novel strategies; optic nerve regeneration; prevent; regenerative; research study; retinal axon; small hairpin RNA; vector

DESCRIPTION (provided by applicant): Injured axons in the mature central nervous system (CNS), including the optic nerve, cannot regenerate spontaneously. This inability to regenerate causes permanent disability after CNS injuries. A better understanding of the impediments to axon regeneration, and novel approaches towards overcoming them, are necessary for the development of new drugs and procedures that may improve the fate of patients with nervous system injury in the future. Our goal is to enable CNS axon regeneration by elevating intrinsic growth signaling. The RAF kinase is known to drive fast axon growth in embryonic sensory neurons; we therefore will now activate this kinase in the retina. Our first aim is to promote regeneration in the injured optic nerve using a conditional B-RAF gain-of-function mouse model. We will then test the roles of signaling molecules downstream of RAF signaling - the MEKs, ERKs and RNDs - for their contributions to B-RAF-driven retinal axon regeneration (Aim 2). Next, we plan to combine activation of B-RAF with activation of PI3-kinase signaling (using a knock-out of the PI3-kinase antagonist PTEN) to see whether this combination will further boost regenerative optic nerve axon growth in vivo (Aim 3). If we can observe regeneration into any of the optic tract nuclei, we will test the mice for any recovery of visual function; such functional recovery being the ultimate goal of all axon regeneration studies. The proposed study will define the roles of RAF signaling and its downstream effectors in the context of optic nerve regeneration, laying groundwork for translational research and for the identification of novel drug targets.

描述（由申请人提供）：包括视神经在内的成熟中枢神经系统（CNS）中受伤的轴突不能自发再生。这种无法再生会导致中枢神经系统受伤后永久残疾。更好地了解轴突再生的障碍，以及克服它们的新方法，对于开发新药和程序的开发是必要的，这些新药和程序可能会改善未来神经系统损伤患者的命运。 我们的目标是通过提高固有生长信号传导来实现CNS轴突再生。已知RAF激酶在胚胎感觉神经元中驱动快速轴突生长。因此，我们现在将在视网膜中激活这种激酶。我们的第一个目的是使用条件B-RAF功能获得的小鼠模型来促进受伤的视神经的再生。然后，我们将测试RAF信号传导下游信号分子的作用 - Meks，Erks和RNDS对B -RAF驱动的视网膜轴突再生的贡献（AIM 2）。接下来，我们计划将B-RAF的激活与PI3-激酶信号传导的激活（使用PI3-激酶拮抗剂PTEN的敲除），以查看这种组合是否会进一步增强体内再生视神经轴突的生长（AIM 3）。如果我们可以观察到任何视频核的再生，我们将测试小鼠的视觉功能的任何恢复。这种功能恢复是所有轴突再生研究的最终目标。 拟议的研究将在视神经再生的背景下定义RAF信号传导及其下游效应子的作用 目标。