Jin Y, Bouyer J, Shumsky J S, Haas C, Fischer I
Department of Neurobiology and Anatomy, Drexel University College of Medicine, Philadelphia PA 19129, United States.
Department of Neurobiology and Anatomy, Drexel University College of Medicine, Philadelphia PA 19129, United States.
Neuroscience. 2016 Apr 21;320:69-82. doi: 10.1016/j.neuroscience.2016.01.066. Epub 2016 Feb 4.
Previous studies demonstrated that neural progenitor cells (NPCs) transplanted into a subacute contusion injury improve motor, sensory, and bladder function. In this study we tested whether transplanted NPCs can also improve functional recovery after chronic spinal cord injury (SCI) alone or in combination with the reduction of glial scar and neurotrophic support. Adult rats received a T10 moderate contusion. Thirteen weeks after the injury they were divided into four groups and received either: 1. Medium (control), 2. NPC transplants, 3. NPC+lentivirus vector expressing chondroitinase, or 4. NPC+lentivirus vectors expressing chondroitinase and neurotrophic factors. During the 8 weeks post-transplantation the animals were tested for functional recovery and eventually analyzed by anatomical and immunohistochemical assays. The behavioral tests for motor and sensory function were performed before and after injury, and weekly after transplantation, with some animals also tested for bladder function at the end of the experiment. Transplant survival in the chronic injury model was variable and showed NPCs at the injury site in 60% of the animals in all transplantation groups. The NPC transplants comprised less than 40% of the injury site, without significant anatomical or histological differences among the groups. All groups also showed similar patterns of functional deficits and recovery in the 12 weeks after injury and in the 8 weeks after transplantation using the Basso, Beattie, and Bresnahan rating score, the grid test, and the Von Frey test for mechanical allodynia. A notable exception was group 4 (NPC together with chondroitinase and neurotrophins), which showed a significant improvement in bladder function. This study underscores the therapeutic challenges facing transplantation strategies in a chronic SCI in which even the inclusion of treatments designed to reduce scarring and increase neurotrophic support produce only modest functional improvements. Further studies will have to identify the combination of acute and chronic interventions that will augment the survival and efficacy of neural cell transplants.
先前的研究表明,将神经祖细胞(NPCs)移植到亚急性挫伤损伤中可改善运动、感觉和膀胱功能。在本研究中,我们测试了移植的NPCs是否也能改善慢性脊髓损伤(SCI)后的功能恢复,无论是单独使用还是与减少胶质瘢痕和神经营养支持相结合。成年大鼠接受T10中度挫伤。损伤13周后,将它们分为四组并分别接受:1. 培养基(对照),2. NPC移植,3. NPC+表达软骨素酶的慢病毒载体,或4. NPC+表达软骨素酶和神经营养因子的慢病毒载体。在移植后的8周内,对动物进行功能恢复测试,并最终通过解剖和免疫组织化学分析进行分析。在损伤前后以及移植后每周进行运动和感觉功能的行为测试,一些动物在实验结束时还进行膀胱功能测试。慢性损伤模型中的移植存活率各不相同,所有移植组中60%的动物在损伤部位发现了NPCs。NPC移植占损伤部位的比例不到40%,各组之间在解剖学或组织学上没有显著差异。使用Basso、Beattie和Bresnahan评分、网格试验和机械性异常性疼痛的Von Frey试验,所有组在损伤后12周和移植后8周也表现出相似的功能缺陷和恢复模式。一个显著的例外是第4组(NPC与软骨素酶和神经营养因子一起),其膀胱功能有显著改善。本研究强调了慢性SCI移植策略面临的治疗挑战,即即使加入旨在减少瘢痕形成和增加神经营养支持的治疗,也只能产生适度的功能改善。进一步的研究将必须确定急性和慢性干预措施的组合,以提高神经细胞移植的存活率和疗效。