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局灶性中风、创伤性脑损伤和脊髓损伤后的基因表达变化。

Gene expression changes after focal stroke, traumatic brain and spinal cord injuries.

作者信息

Carmichael S Thomas

机构信息

Department of Neurology, David Geffen School of Medicine at UCLA, Los Angeles, CA 90095, USA.

出版信息

Curr Opin Neurol. 2003 Dec;16(6):699-704. doi: 10.1097/01.wco.0000102621.38669.77.

Abstract

PURPOSE OF REVIEW

Large-scale gene expression profiling has recently been performed on stroke and spinal cord injuries. These studies provide insights into coordinated patterns of gene expression within the injury and the interrelationships of neurodegenerative and neural repair processes after injury.

RECENT FINDINGS

The molecular signals for post-stroke angiogenesis begin within hours of initial cerebral ischemia, with sequential increases in message for initially destabilizing combinations of vascular growth factors and growth factor receptors, followed by growth factor combinations that promote endothelial cell division and stabilization. The overlap in molecular signaling between post-stroke angiogenesis, neurogenesis and axonal sprouting suggests a continuum of vascular and neural reorganization in the tissue adjacent to stroke. Inflammation after injury extends through early and late changes in the cytokine message. SOCS-3, a negative regulator of cytokine signaling, is increased after injury and may be neuroprotective. Components of an adult neuronal growth program have been identified in the peripheral nervous system during axonal regeneration, with overlap to axonal sprouting after stroke. The gene expression profile of the aged brain suggests an altered central nervous system environment that may exacerbate initial injury and impair neural reorganization after stroke and spinal cord injury.

SUMMARY

When rigorously tested and independently validated, data from large-scale gene expression analyses provide new insights into the aggregate genetic control of stroke and spinal cord injury, and the interrelationship of important cellular events within the damaged region. These data also highlight novel genes in these processes, and suggest new directions in the investigation of tissue reorganization and repair after central nervous system injury.

摘要

综述目的

最近对中风和脊髓损伤进行了大规模基因表达谱分析。这些研究为损伤内基因表达的协调模式以及损伤后神经退行性变和神经修复过程的相互关系提供了见解。

最新发现

中风后血管生成的分子信号在最初脑缺血数小时内就开始出现,先是血管生长因子和生长因子受体的不稳定组合的信息依次增加,随后是促进内皮细胞分裂和稳定的生长因子组合。中风后血管生成、神经发生和轴突发芽之间分子信号的重叠表明中风邻近组织中血管和神经重组具有连续性。损伤后的炎症贯穿细胞因子信息的早期和晚期变化。细胞因子信号转导的负调节因子SOCS-3在损伤后增加,可能具有神经保护作用。在轴突再生过程中,已在外周神经系统中鉴定出成年神经元生长程序的组成部分,与中风后的轴突发芽有重叠。老年大脑的基因表达谱表明中枢神经系统环境发生改变,这可能会加重中风和脊髓损伤后的初始损伤并损害神经重组。

总结

经过严格测试和独立验证后,大规模基因表达分析的数据为中风和脊髓损伤的总体遗传控制以及受损区域内重要细胞事件的相互关系提供了新见解。这些数据还突出了这些过程中的新基因,并为中枢神经系统损伤后组织重组和修复的研究指明了新方向。

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