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首页> 外文期刊>Gene therapy >Adenoviral gene transfer of bone morphogenetic protein-7 enhances functional recovery after sciatic nerve injury in rats.
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Adenoviral gene transfer of bone morphogenetic protein-7 enhances functional recovery after sciatic nerve injury in rats.

机译:骨形态发生蛋白7的腺病毒基因转移可增强大鼠坐骨神经损伤后的功能恢复。

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Bone morphogenetic proteins (BMPs), members of the transforming growth factor-beta subfamily, function as instructive signals for neuronal lineage commitment and promote neuronal differentiation. However, the mechanism of BMP7 action in vivo after peripheral nerve injury is poorly understood. This study examines the efficacy of gene transfer of adenoviral (Ad) BMP7 on peripheral neuropathy. Transgene expression was found in both Ad-infected sciatic nerves and their respective remote neurons, indicating Ad transduction by a retrograde transport. After AdBMP7 infection to nerves, the sciatic nerves were crushed or transected. Hind limb functional behavior, including rotarod test and sciatic functional index, were conducted in rats weekly after nerve injury. Interestingly, enhanced BMP7 expression significantly improved hind limb functional recovery in AdBMP7-transduced rats when compared with AdGFP-transduced nerve-crushed or transected rats. Furthermore, AdBMP7 transduction reduced injury-induced macrophage activation, nerve demyelination and axonal degeneration. By contrast, AdBMP7 infection did not affect the hyperalgesia paw-withdrawal latency after nerve injury. We further examined the effect of AdBMP7 infection on sciatic nerve explant and Schwann cell cultures. Enhanced cell proliferation was significantly increased by AdBMP7 transduction in both cultures. Taken together, BMP7 overexpression by Ad gene transfer was beneficial in both nerves and Schwann cells on functional recovery after sciatic nerve injury in rats.
机译:骨形态发生蛋白(BMP)是转化生长因子-β亚家族的成员,可作为神经元谱系定型的指导信号并促进神经元分化。然而,人们对外周神经损伤后体内BMP7作用的机制了解甚少。这项研究检查了腺病毒(Ad)BMP7基因转移对周围神经病变的疗效。在感染Ad的坐骨神经和它们各自的远端神经元中均发现了转基因表达,表明通过逆行转运进行Ad转导。 AdBMP7感染神经后,坐骨神经被压扁或切断。神经损伤后每周在大鼠中进行后肢功能行为,包括旋转脚踏试验和坐骨神经功能指数。有趣的是,与AdGFP转导的神经粉碎或横断大鼠相比,增强的BMP7表达显着改善了AdBMP7转导的大鼠的后肢功能恢复。此外,AdBMP7转导减少了损伤诱导的巨噬细胞活化,神经脱髓鞘和轴突变性。相比之下,AdBMP7感染并不影响神经损伤后痛觉过敏的爪撤回潜伏期。我们进一步检查了AdBMP7感染对坐骨神经外植体和施万细胞培养的影响。在两种培养物中,AdBMP7转导都显着增强了细胞增殖。两者合计,通过Ad基因转移的BMP7过表达对大鼠坐骨神经损伤后的神经和雪旺细胞功能恢复均有益。

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