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经基因改造以表达脑源性神经营养因子(BDNF)的成纤维细胞移植可促进成年大鼠红核脊髓轴突的再生和前肢功能的恢复。

Transplants of fibroblasts genetically modified to express BDNF promote regeneration of adult rat rubrospinal axons and recovery of forelimb function.

作者信息

Liu Y, Kim D, Himes B T, Chow S Y, Schallert T, Murray M, Tessler A, Fischer I

机构信息

Department of Neurobiology and Anatomy, Medical College of Pennsylvania/Hahnemann University, Philadelphia, Pennsylvania 19129, USA.

出版信息

J Neurosci. 1999 Jun 1;19(11):4370-87. doi: 10.1523/JNEUROSCI.19-11-04370.1999.

Abstract

Adult mammalian CNS neurons do not normally regenerate their severed axons. This failure has been attributed to scar tissue and inhibitory molecules at the injury site that block the regenerating axons, a lack of trophic support for the axotomized neurons, and intrinsic neuronal changes that follow axotomy, including cell atrophy and death. We studied whether transplants of fibroblasts genetically engineered to produce brain-derived neurotrophic factor (BDNF) would promote rubrospinal tract (RST) regeneration in adult rats. Primary fibroblasts were modified by retroviral-mediated transfer of a DNA construct encoding the human BDNF gene, an internal ribosomal entry site, and a fusion gene of lacZ and neomycin resistance genes. The modified fibroblasts produce biologically active BDNF in vitro. These cells were grafted into a partial cervical hemisection cavity that completely interrupted one RST. One and two months after lesion and transplantation, RST regeneration was demonstrated with retrograde and anterograde tracing techniques. Retrograde tracing with fluorogold showed that approximately 7% of RST neurons regenerated axons at least three to four segments caudal to the transplants. Anterograde tracing with biotinylated dextran amine revealed that the RST axons regenerated through and around the transplants, grew for long distances within white matter caudal to the transplant, and terminated in spinal cord gray matter regions that are the normal targets of RST axons. Transplants of unmodified primary fibroblasts or Gelfoam alone did not elicit regeneration. Behavioral tests demonstrated that recipients of BDNF-producing fibroblasts showed significant recovery of forelimb usage, which was abolished by a second lesion that transected the regenerated axons.

摘要

成年哺乳动物的中枢神经系统(CNS)神经元通常不会再生其被切断的轴突。这种再生失败被归因于损伤部位的瘢痕组织和抑制性分子,它们会阻碍再生轴突;轴突切断的神经元缺乏营养支持;以及轴突切断后神经元内在的变化,包括细胞萎缩和死亡。我们研究了经基因工程改造以产生脑源性神经营养因子(BDNF)的成纤维细胞移植是否会促进成年大鼠红核脊髓束(RST)的再生。通过逆转录病毒介导的DNA构建体转移来修饰原代成纤维细胞,该构建体编码人BDNF基因、一个内部核糖体进入位点以及lacZ和新霉素抗性基因的融合基因。修饰后的成纤维细胞在体外产生具有生物活性的BDNF。将这些细胞移植到部分颈半切腔中,该腔完全中断了一条RST。在损伤和移植后的1个月和2个月,通过逆行和顺行示踪证明了RST的再生。用荧光金进行逆行示踪显示,约7%的RST神经元在移植部位尾侧至少三到四个节段处再生了轴突。用生物素化葡聚糖胺进行顺行示踪表明,RST轴突通过移植部位并在其周围再生,在移植部位尾侧的白质中长距离生长,并终止于RST轴突的正常靶标脊髓灰质区域。未修饰的原代成纤维细胞或单独的明胶海绵移植均未引发再生。行为测试表明,接受产生BDNF的成纤维细胞移植的大鼠前肢使用情况有显著恢复,而横断再生轴突的第二次损伤消除了这种恢复。

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