首页> 外文期刊>Gene therapy >Attenuation of ganglioside GM1 accumulation in the brain of GM1 gangliosidosis mice by neonatal intravenous gene transfer.
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Attenuation of ganglioside GM1 accumulation in the brain of GM1 gangliosidosis mice by neonatal intravenous gene transfer.

机译:新生儿静脉内基因转移可减轻GM1神经节病小鼠大脑中神经节苷脂GM1的积累。

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摘要

A single intravenous injection with 4 x 10(7) PFU of recombinant adenovirus encoding mouse beta-galactosidase cDNA to newborn mice provided widespread increases of beta-galactosidase activity, and attenuated the development of the disease including the brain at least for 60 days. The beta-galactosidase activity showed 2-4 times as high a normal activity in the liver and lung, and 50 times in the heart. In the brain, while the activity was only 10-20% of normal, the efficacy of the treatment was distinct. At the 30th day after the injection, significant attenuation of ganglioside GM1 accumulation in the cerebrum was shown in three out of seven mice. At the 60th day after the injection, the amount of ganglioside GM1 was above the normal range in all treated mice, which was speculated to be the result of reaccumulation. However, the values were still definitely lower in most of the treated mice than those in untreated mice. In the histopathological study, X-gal-positive cells, which showed the expression of exogenous beta-galactosidase gene, were observed in the brain. It is noteworthy that neonatal administration via blood vessels provided access to the central nervous system because of the incompletely formed blood-brain barrier.
机译:向新生小鼠单次静脉内注射4 x 10(7)PFU编码小鼠β-半乳糖苷酶cDNA的重组腺病毒,可大大增加β-半乳糖苷酶的活性,并至少在60天内减弱了包括大脑在内的疾病的发展。 β-半乳糖苷酶的活性在肝和肺中显示为正常活性的2-4倍,在心脏中显示为50倍。在大脑中,尽管活性仅为正常水平的10-20%,但治疗效果却很明显。注射后第30天,在七只小鼠中,有三只显示出神经节苷脂GM1在大脑中的积累明显减少。注射后第60天,神经节苷脂GM1的量在所有治疗的小鼠中均高于正常范围,这被认为是重新蓄积的结果。但是,在大多数治疗小鼠中,该值仍肯定低于未治疗小鼠中的值。在组织病理学研究中,在大脑中观察到X-gal阳性细胞,该细胞显示外源性β-半乳糖苷酶基因的表达。值得注意的是,由于未完全形成血脑屏障,因此通过血管进行新生儿给药可进入中枢神经系统。

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