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首页> 外文期刊>Molecular therapy: the journal of the American Society of Gene Therapy >Neurotensin polyplex as an efficient carrier for delivering the human GDNF gene into nigral dopamine neurons of hemiparkinsonian rats.
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Neurotensin polyplex as an efficient carrier for delivering the human GDNF gene into nigral dopamine neurons of hemiparkinsonian rats.

机译:神经降压素复合物作为将人GDNF基因传递到半帕金森病大鼠的黑色多巴胺神经元中的有效载体。

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摘要

Recently we showed that the neurotensin polyplex is a nanoparticle carrier system that targets reporter genes in nigral dopamine neurons in vivo. Herein, we report its first practical application in experimental parkinsonism, which consisted of transfecting dopamine neurons with the gene coding for human glial cell line-derived neurotrophic factor (hGDNF). Hemiparkinsonism was induced in rats by a single dose of 6-hydroxydopamine (30 microg) into the ventrolateral part of the striatum. We showed that transfection of the hGDNF gene into the substantia nigra of rats 1 week after the neurotoxin injection produced biochemical, anatomical, and functional recovery from hemiparkinsonism. RT-PCR analysis showed mRNA expression of exogenous hGDNF in the transfected substantia nigra. Western blot analysis verified transgene expression by recognizing the flag epitope added at the C-terminus of the hGDNF polypeptide, which was found mainly in dopamine neurons by double immunofluorescence techniques. These data indicate that the neurotensin polyplex holds great promise for the neuroprotective therapy of Parkinson disease.
机译:最近,我们发现神经降压素复合物是一种纳米颗粒载体系统,在体内靶向黑质多巴胺神经元中的报告基因。在本文中,我们报告了其在实验性帕金森病中的首次实际应用,该试验包括用编码人胶质细胞源性神经营养因子(hGDNF)的基因转染多巴胺神经元。在大鼠的纹状体腹侧部分单剂量6-羟基多巴胺(30微克)可诱发半帕金森综合症。我们显示神经毒素注射后1周,将hGDNF基因转染到大鼠的黑质中,产生了从半帕金森氏反应的生化,解剖学和功能恢复。 RT-PCR分析显示外源hGDNF在转染黑质中的mRNA表达。 Western blot分析通过识别在hGDNF多肽C端添加的标志抗原决定簇来验证转基因表达,该抗原决定簇主要是通过双重免疫荧光技术在多巴胺神经元中发现的。这些数据表明神经降压素复合物对于帕金森氏病的神经保护治疗具有广阔的前景。

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