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Distribution and anti-HBV effects of antisense oligodeoxynu-cleotides conjugated to galactosylated poly-L-lysine

机译:反义寡聚脱氧核糖核酸与半乳糖基化聚-L-赖氨酸结合的分布和抗HBV作用

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AIM: To describe distribution of the phosphorothioated antisense oligodeoxynucleotides (PS-asODNs) conjugated to galactosylated poly-L-lysine (Gal-PLL) in mice, and to observe their effects on expression of HBV gene in the 2.2. 15 cells and transgenic mice. METHODS: According to the result of direct sequencing of PCR amplified products, a 16 mer phosphorothioate analogue of the antisense oligodeoxynucleotides (PS-asODNs) directed against the HBV U_5-like region was conjugated to the hepatotropic Gal-PLL molecules. Its distribution was demonstrated using asODNs labeled with ~(32)P at the 5′ terminus with a T4-polynucleotide Kinase. Its inhibition effect on HBV expression was observed in the transfected 2.2.15 cells and transgenic mice. RESULTS: The Gal-PLL and asODNs could form stable complex at a molar ratio of 2:1. As shown in the HBV-transfected 2.2.15 cells, the inhibition effects of asODNs alone and asODNs conjugated to Gal-PLL, at 10 μmol/L for both, on HBsAg and HBeAg production were different,the former being 70% and 58%, respectively, and the latter being 96% and 82%, respectively. A more pronounced reduction was also observed in viral DNA load in the culture supernatant for the test with Gal-PLL-asODNs. Among many mouse organs, livers retained more asODNs molecules after administration. The preferential concentration in liver was found to be 52.14% for Gal-PLL-asODNs, as high as 2.38-fold of that for asODNs (21.9%). Both elements decreased gradually in liver, with 2.9% of the former, 5.99% of the latter retained 24 hours after the administration. The injection interval, therefore, was recommended to be 24 hours. In the transgenic mice, serum HBsAg decreased significantly (P<0.01) at the 12th day after administrating Gal-PLL- asODNs, the serum HBV DNA turned negative in 4 of the 6 mice. CONCLUSION: Antisense oligodeoxynucleotides conjugated to Gal-PLL can be concentrated in liver and intaked by hepatocytic cells. This may result in specific inhibition of expression and replication of HBV in vitro and in vivo.
机译:目的:描述与半乳糖基化聚L-赖氨酸(Gal-PLL)结合的硫代磷酸化反义寡聚脱氧核苷酸(PS-asODNs)在小鼠中的分布,并观察其对2.2中HBV基因表达的影响。 15个细胞和转基因小鼠。方法:根据PCR扩增产物的直接测序结果,将针对HBV U_5样区域的反义寡脱氧核苷酸(PS-asODNs)的16聚体硫代磷酸酯类似物与促肝Gal-PLL分子缀合。使用带有T4多核苷酸激酶的5'末端标记有〜(32)P的asODN证实了其分布。在转染的2.2.15细胞和转基因小鼠中观察到其对HBV表达的抑制作用。结果:Gal-PLL和asODN可以摩尔比为2:1形成稳定的配合物。如转染HBV的2.2.15细胞中所示,单独的asODNs和与Gal-PLL偶联的asODNs在10μmol/ L时对HBsAg和HBeAg产生的抑制作用不同,前者分别为70%和58%分别为96%和82%。对于用Gal-PLL-asODNs进行的测试,在培养上清液中的病毒DNA负载也观察到了更明显的降低。在许多小鼠器官中,给药后肝脏保留了更多的asODNs分子。发现Gal-PLL-asODNs在肝脏中的优先浓度为52.14%,是asODNs(21.9%)的2.38倍。两种元素在肝脏中均逐渐降低,前者为2.9%,后者为5.99%,在给药后24小时保留。因此,建议注射间隔为24小时。在转基因小鼠中,给予Gal-PLL-asODNs后第12天,血清HBsAg显着降低(P <0.01),这6只小鼠中有4只的血清HBV DNA变为阴性。结论:与Gal-PLL结合的反义寡聚脱氧核苷酸可以在肝脏中浓缩,并被肝细胞摄取。这可能导致在体外和体内特异性抑制HBV的表达和复制。

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