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采用联合策略可提高雪旺细胞移植对脊髓修复的疗效。

Efficacy of Schwann cell transplantation for spinal cord repair is improved with combinatorial strategies.

作者信息

Bunge Mary Bartlett

机构信息

The Miami Project to Cure Paralysis, University of Miami Miller School of Medicine, 1095 NW 14th Terrace, Miami, FL, 33136, USA.

出版信息

J Physiol. 2016 Jul 1;594(13):3533-8. doi: 10.1113/JP271531. Epub 2016 May 10.

Abstract

When cells (including Schwann cells; SCs) of the peripheral nervous system (PNS) could be purified and expanded in number in tissue culture, Richard Bunge in 1975 envisioned that the SCs could be introduced to repair the central nervous system (CNS), as SCs enable axons to regenerate after PNS injury. Importantly, autologous human SCs could be transplanted into injured human spinal cord. Availability of the new culture systems to study interactions between sensory neurons, SCs and fibroblasts increased our knowledge of SC biology in the 1970s and '80s. Joining the Miami Project to Cure Paralysis in 1989 brought the opportunity to use this knowledge to initiate spinal cord repair studies. Development of a rat complete spinal cord transection/SC bridge model allowed the demonstration that axons regenerate into the SC bridge. Together with study of contused rat spinal cord, it was concluded that implanted SCs reduce cavitation, protect tissue around the lesion, support axon regeneration and form myelin. SC transplantation efficacy was improved when combined with neurotrophins, elevation of cyclic AMP levels, olfactory ensheathing cells, a steroid or chondroitinase. Increased efficacy meant higher numbers of axons, particularly from the brainstem, and more SC-myelinated axons in the implants and improvement in hindlimb movements. Human SCs support axon regeneration as do rat SCs. Astrocytes at the SC bridge-host spinal cord interfaces play a key role in determining whether axons enter the SC milieu. The SC work described here contributed to gaining approval from the FDA for an initial autologous human SC clinical trial (at the Miami Project) that has been completed and found to be safe.

摘要

当外周神经系统(PNS)的细胞(包括雪旺细胞;SCs)能够在组织培养中被纯化并大量扩增时,理查德·邦奇在1975年设想,可以引入雪旺细胞来修复中枢神经系统(CNS),因为雪旺细胞能使PNS损伤后的轴突再生。重要的是,自体人类雪旺细胞可以移植到受伤的人类脊髓中。20世纪70年代和80年代,新的培养系统用于研究感觉神经元、雪旺细胞和成纤维细胞之间的相互作用,这增加了我们对雪旺细胞生物学的了解。1989年加入迈阿密瘫痪治疗项目带来了利用这一知识启动脊髓修复研究的机会。大鼠完全脊髓横断/雪旺细胞桥模型的建立使得能够证明轴突可以再生进入雪旺细胞桥。结合对挫伤大鼠脊髓的研究,得出的结论是,植入的雪旺细胞可减少空洞形成,保护损伤周围组织,支持轴突再生并形成髓鞘。当与神经营养因子、环磷酸腺苷水平升高、嗅鞘细胞、类固醇或软骨素酶联合使用时,雪旺细胞移植效果得到改善。效果的提高意味着轴突数量增加,特别是来自脑干的轴突,植入物中雪旺细胞髓鞘化的轴突增多,后肢运动也有所改善。人类雪旺细胞与大鼠雪旺细胞一样支持轴突再生。雪旺细胞桥与宿主脊髓界面处的星形胶质细胞在决定轴突是否进入雪旺细胞环境中起关键作用。这里描述的雪旺细胞研究工作促成了美国食品药品监督管理局(FDA)批准了一项初步的自体人类雪旺细胞临床试验(在迈阿密项目中),该试验已经完成且结果显示是安全的。

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