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首页> 外文期刊>Brain research bulletin >Peripheral and mesencephalic transfer of a synthetic gene for the thymic peptide thymulin.
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Peripheral and mesencephalic transfer of a synthetic gene for the thymic peptide thymulin.

机译:胸腺肽胸腺肽合成基因的外周和中脑转移。

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Thymulin is a thymic peptide with antiinflammatory activity in the brain. We constructed a recombinant adenoviral vector, RAd-FTS, expressing a synthetic DNA sequence encoding met-FTS, a biologically active analog of thymulin and used it for peripheral and central gene transfer in rats. Thymulin concentration in serum and brain tissue was determined by bioassay. Reporter gene expression in the substantia nigra (SN) was quantitated by enzymohistochemistry or fluorescence microscopy using an appropriate image analysis software. A single intramuscular injection (10(8) plaque forming units (pfu)/animal) of RAd-FTS in thymectomized rats (nondetectable serum thymulin) induced supraphysiologic serum thymulin levels for at least 110 days (123+/-22 fg/ml versus 598+/-144 fg/ml in intact and vector-injected rats, respectively). Stereotaxic intranigral injection of RAd-FTS induced steady expression levels of met-FTS for at least 90 days, whereas expression of adenovirally transferred reporter genes coding for green fluorescent protein fused to HSV thymidine kinase (GFP-TK)(fus) or E.coli beta-galactosidase (beta-gal), declined drastically within a month (% transgene expression in the SN on post-injection day 30 relative to day 2 was: 18, <1 and 125%, for beta-gal, (GFP-TK)(fus) and met-FTS, respectively). We conclude that RAd-FTS constitutes a suitable biotechnological tool for the assessment of peripheral and central thymulin gene therapy in animal models of nigral dopaminergic neurodegeneration induced by pro-inflammatory agents.
机译:胸腺素是在大脑中具有抗炎活性的胸腺肽。我们构建了重组腺病毒载体RAd-FTS,该载体表达编码met-FTS(胸腺素的生物活性类似物)的合成DNA序列,并将其用于大鼠的外周和中枢基因转移。通过生物测定法测定血清和脑组织中的Thymulin浓度。使用适当的图像分析软件,通过酶组织化学或荧光显微镜术对黑质(SN)中报告基因的表达进行定量。在胸腺切除的大鼠(不可检测的血清胸腺素)中单次肌肉注射(10(8)斑块形成单位(pfu)/动物)RAd-FTS诱导超生理性血清胸腺素水平至少持续110天(123 +/- 22 fg / ml,而在完整和载体注射的大鼠中分别为598 +/- 144 fg / ml)。立体定向鼻内注射RAd-FTS诱导稳定表达水平的met-FTS至少90天,而腺病毒转移的报告基因的表达编码与HSV胸苷激酶(GFP-TK)(fus)或大肠杆菌融合的绿色荧光蛋白β-半乳糖苷酶(beta-gal),在一个月内急剧下降(注射后第30天相对于第2天,SN中转基因表达的百分比为:对于β-gal,(GFP-TK为18,<1和125% )(fus)和met-FTS)。我们得出的结论是,RAd-FTS构成了一种合适的生物技术工具,用于评估由促炎剂引起的黑质多巴胺能神经退行性动物模型中的外周和中枢胸腺素基因治疗。

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