首页> 外文期刊>European journal of pain : >Subarachnoid transplantation of immortalized galanin-overexpressing astrocytes attenuates chronic neuropathic pain.
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Subarachnoid transplantation of immortalized galanin-overexpressing astrocytes attenuates chronic neuropathic pain.

机译:永生化的甘丙肽过表达星形胶质细胞的蛛网膜下腔移植减轻了慢性神经性疼痛。

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Treatment of chronic neuropathic pain resulted from peripheral nerve injury is one of the most difficult problems in modern clinical practice. The use of cell lines as biologic "minipumps" to chronically deliver anti-nociceptive molecules into the pain-processing centers of spinal cord is a newly developing technique for the treatment of pain. Moreover, spinal administration of exogenous galanin (GAL) is a useful target for the treatment of chronic pain after nerve injury. Because of better histocompatibility, lower immunogenicity and reproducibility, immortalized astrocytes (IAST) have been served as a promising cellular vehicle to deliver therapeutic molecules into CNS. In this study, the rat IAST was transfected with rat preprogalanin cDNA and the galanin-synthesizing and secreting cell line, IAST/GAL, was isolated. After cells were transplanted into the subarachnoid space of rats with chronic neuropathic pain induced by spared nerve injury (SNI) of sciatic nerve, their analgesic potential was evaluated by behavioral tests. The results showed that IAST/GAL transfected with preprogalanin gene could express and secrete significantly higher level of GAL protein in vitro and in vivo as compared with control cells. In addition, the pain-related behaviors, thermal hyperalgesia and mechanical allodynia were significantly alleviated during the 1-7 weeks after grafts of IAST/GAL cells, which could be reversed by galanin receptor antagonist M35 temporarily. Taken together, these data suggest that subarachnoid transplant of immortalized galanin-overexpressing astrocytes near the pain-processing centers was able to reverse the development of chronic neuropathic pain, which offers an adjunct approach to currently used therapies for the pain management.
机译:由周围神经损伤引起的慢性神经性疼痛的治疗是现代临床实践中最困难的问题之一。使用细胞系作为生物“小动物”来将抗伤害感受性分子长期传递到脊髓的疼痛处理中心是一种新的治疗疼痛的技术。而且,脊柱施用外源甘丙肽(GAL)是治疗神经损伤后慢性疼痛的有用靶标。由于更好的组织相容性,较低的免疫原性和可重复性,永生化的星形胶质细胞(IAST)已被用作将治疗性分子递送到CNS的有前途的细胞载体。在这项研究中,大鼠IAST已被大鼠前普兰蛋白原cDNA转染,并分离了甘丙肽合成和分泌细胞系IAST / GAL。将细胞移植到坐骨神经多余神经损伤(SNI)所致的慢性神经性疼痛大鼠的蛛网膜下腔中,通过行为测试评估其镇痛潜力。结果表明,与对照细胞相比,转染前普拉加林原基因的IAST / GAL可以在体内外表达和分泌更高水平的GAL蛋白。此外,在IAST / GAL细胞移植后的1-7周内,与疼痛相关的行为,热痛觉过敏和机械性异常性疼痛得到了明显缓解,甘丙肽受体拮抗剂M35可以暂时逆转这种情况。综上所述,这些数据表明在疼痛处理中心附近的永生化的甘丙肽过表达星形胶质细胞的蛛网膜下移植能够逆转慢性神经性疼痛的发展,这为目前用于疼痛管理的疗法提供了辅助方法。

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