Yoshihara Hiroyuki, Shumsky Jed S, Neuhuber Birgit, Otsuka Takanobu, Fischer Itzhak, Murray Marion
Department of Neurobiology and Anatomy, Drexel University College of Medicine, Philadelphia, PA 19129, USA.
Brain Res. 2006 Nov 13;1119(1):65-75. doi: 10.1016/j.brainres.2006.08.080. Epub 2006 Oct 6.
Previous studies have demonstrated that either transplantation of bone marrow stromal cells (MSC) or physical exercise regimens can elicit limited functional recovery following spinal cord injury, presumably through different mechanisms. The present study examined whether transplantation of MSC derived from transgenic Fischer alkaline phosphatase (AP) rats, in combination with exercise, would have synergistic effects leading to recovery of function that is greater than either alone. Adult female Sprague-Dawley rats received a moderate thoracic contusion injury and were divided into three groups: operated controls (Op-Control), MSC transplant recipients (MSC), and MSC transplant recipients plus exercise (MSC+Ex). Nine days after contusion, a Vitrogen matrix +/-one million MSC was injected into the lesion site in all animals. Immunosuppression with high doses of Cyclosporine A, required for MSC survival, was provided for all animals. Passive hindlimb exercise on motorized bicycles was applied 1 h/day, 3 days/week to the MSC+Ex group. A battery of behavioral tests was performed weekly to assess motor and sensory functions in all 3 groups for 12 weeks. Morphological evaluation included MSC survival, evidence of axonal growth into grafts, phenotypic analysis of MSC, and lesion/transplant size. The weight of the medial gastrocnemius muscle, a hindlimb muscle activated during stance, was used to identify extent of atrophy. No differences in motor recovery were found among the three groups. MSC survived 3 months after transplantation, indicating that the immunosuppression treatment was successful. The extent of survival was variable, and there was no correlation between MSC survival and behavioral scores. The matrix persisted, filling the lesion cavity, and some axons grew into the lesion/matrix but to a similar extent in all groups. There was no difference in lesion/matrix size among groups, indicating no neuroprotective effect on the host provided by the treatments. Immunocytochemical analysis provided no evidence that MSC differentiated into neurons, astrocytes or oligodendrocytes. Muscle mass of the medial gastrocnemius was diminished in the Op-Control group indicating significant atrophy, but was partially preserved in both the MSC and MSC+Ex groups. Our results indicate that combining the beneficial effects of rat MSC and this exercise protocol was not sufficient to enhance behavioral recovery.
先前的研究表明,骨髓基质细胞(MSC)移植或体育锻炼方案均可在脊髓损伤后引发有限的功能恢复,推测其机制不同。本研究探讨了源自转基因Fischer碱性磷酸酶(AP)大鼠的MSC移植联合运动是否会产生协同效应,从而导致功能恢复程度大于单独使用其中任何一种方法。成年雌性Sprague-Dawley大鼠接受中度胸椎挫伤,并分为三组:手术对照组(Op-Control)、MSC移植受体组(MSC)和MSC移植受体加运动组(MSC+Ex)。挫伤9天后,向所有动物的损伤部位注射含或不含100万个MSC的Vitrogen基质。所有动物均接受高剂量环孢素A免疫抑制,这是MSC存活所必需的。MSC+Ex组每周3天、每天1小时在电动自行车上进行被动后肢运动。每周进行一系列行为测试,持续12周,以评估所有三组的运动和感觉功能。形态学评估包括MSC存活情况、轴突长入移植物的证据、MSC的表型分析以及损伤/移植大小。腓肠肌内侧肌的重量(一种在站立时被激活的后肢肌肉)用于确定萎缩程度。三组之间在运动恢复方面未发现差异。MSC在移植后存活了3个月,表明免疫抑制治疗成功。存活程度存在差异,且MSC存活与行为评分之间无相关性。基质持续存在,填充损伤腔,一些轴突长入损伤/基质,但在所有组中的程度相似。各组之间损伤/基质大小无差异,表明这些治疗方法对宿主没有神经保护作用。免疫细胞化学分析未提供证据表明MSC分化为神经元、星形胶质细胞或少突胶质细胞。Op-Control组腓肠肌内侧肌质量减少,表明有明显萎缩,但在MSC组和MSC+Ex组中部分得以保留。我们的结果表明,将大鼠MSC的有益作用与该运动方案相结合不足以增强行为恢复。
