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斑马鱼视神经再生过程中眼睛基因表达模式的时间进程分析

Time Course Analysis of Gene Expression Patterns in Zebrafish Eye During Optic Nerve Regeneration.

作者信息

McCurley Amy T, Callard Gloria V

机构信息

Department of Biology, Boston University, 5 cummington street, Boston, MA 02215 USA.

出版信息

J Exp Neurosci. 2010 Jul 13;2010(4):17-33.

Abstract

It is well-established that neurons in the adult mammalian central nervous system (CNS) are terminally differentiated and, if injured, will be unable to regenerate their connections. In contrast to mammals, zebrafish and other teleosts display a robust neuroregenerative response. Following optic nerve crush (ONX), retinal ganglion cells (RGC) regrow their axons to synapse with topographically correct targets in the optic tectum, such that vision is restored in approximately 21 days. What accounts for these differences between teleostean and mammalian responses to neural injury is not fully understood. A time course analysis of global gene expression patterns in the zebrafish eye after ONX can help to elucidate cellular and molecular mechanisms that contribute to a successful neuroregeneration. To define different phases of regeneration after ONX, alpha tubulin 1 (tuba1) and growth-associated protein 43 (gap43), markers previously shown to correspond to morphophological events, were measured by real time quantitative PCR (qPCR). Microarray analysis was then performed at defined intervals (6 hours, 1, 4, 12, and 21 days) post-ONX and compared to SHAM. Results show that optic nerve damage induces multiple, phase-related transcriptional programs, with the maximum number of genes changed and highest fold-change occurring at 4 days. Several functional groups affected by optic nerve regeneration, including cell adhesion, apoptosis, cell cycle, energy metabolism, ion channel activity, and calcium signaling, were identified. Utilizing the whole eye allowed us to identify signaling contributions from the vitreous, immune and glial cells as well as the neural cells of the retina. Comparisons between our dataset and transcriptional profiles from other models of regeneration in zebrafish retina, heart and fin revealed a subset of commonly regulated transcripts, indicating shared mechanisms in different regenerating tissues. Knowledge of gene expression patterns in all components of the eye in a model of successful regeneration provides an entry point for functional analyses, and will help in devising hypotheses for testing normal and toxic regulatory factors.

摘要

众所周知,成年哺乳动物中枢神经系统(CNS)中的神经元是终末分化的,一旦受损,将无法再生其连接。与哺乳动物不同,斑马鱼和其他硬骨鱼表现出强大的神经再生反应。视神经挤压(ONX)后,视网膜神经节细胞(RGC)会重新生长其轴突,与视顶盖中拓扑结构正确的靶标形成突触,从而在大约21天内恢复视力。硬骨鱼和哺乳动物对神经损伤反应的这些差异的原因尚未完全了解。对ONX后斑马鱼眼睛中全局基因表达模式的时间进程分析有助于阐明促成成功神经再生的细胞和分子机制。为了定义ONX后再生的不同阶段,通过实时定量PCR(qPCR)测量了先前显示与形态学事件相对应的标记物α微管蛋白1(tuba1)和生长相关蛋白43(gap43)。然后在ONX后的特定时间间隔(6小时、1天、4天、12天和21天)进行微阵列分析,并与假手术组进行比较。结果表明,视神经损伤诱导了多个与阶段相关的转录程序,在4天时基因变化数量最多且倍数变化最高。确定了受视神经再生影响的几个功能组,包括细胞粘附、细胞凋亡、细胞周期、能量代谢、离子通道活性和钙信号传导。利用整个眼睛使我们能够确定玻璃体、免疫和神经胶质细胞以及视网膜神经细胞的信号贡献。我们的数据集与斑马鱼视网膜、心脏和鳍的其他再生模型的转录谱之间的比较揭示了一组共同调控的转录本,表明不同再生组织中存在共同机制。了解成功再生模型中眼睛所有成分的基因表达模式为功能分析提供了切入点,并将有助于设计用于测试正常和毒性调节因子的假设。

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