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DNA vaccines expressing the duck hepatitis B virus surface proteins lead to reduced numbers of infected hepatocytes and protect ducks against the development of chronic infection in a virus dose-dependent manner

机译:表达鸭乙型肝炎病毒表面蛋白的DNa疫苗导致感染的肝细胞数量减少,并以病毒剂量依赖性方式保护鸭免受慢性感染的发展

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摘要

We tested the efficacy of DNA vaccines expressing the duck hepatitis B virus (DHBV) pre-surface (pre-S/S) and surface (S) proteins in modifying the outcome of infection in 14-day-old ducks. In two experiments, Pekin Aylesbury ducks were vaccinated on days 4 and 14 of age with plasmid DNA vaccines expressing either the DHBV pre-S/S or S proteins, or the control plasmid vector, pcDNA1.1Amp. All ducks were then challenged intravenously on day 14 of age with 5 x 10(7) or 5 x 10(8) DHBV genomes. Levels of initial DHBV infection were assessed using liver biopsy tissue collected at day 4 post-challenge (p.c.) followed and immunostained for DHBV surface antigen to determine the percentage of infected hepatocytes. All vector vaccinated ducks challenged with 5 x 10(7) and 5 x 10(8) DHBV genomes had an average of 3.21% and 20.1% of DHBV-positive hepatocytes respectively at day 4 p.c. and 16 out of 16 ducks developed chronic DHBV infection. In contrast, pre-S/S and S vaccinated ducks challenged with 5 x 10(7) DHBV genomes had reduced levels of initial infection with an average of 1.38% and 1.93% of DHBV-positive hepatocytes at day 4 p.c. respectively and 10 of 18 ducks were protected against chronic infection. The pre-S/S and the S DNA vaccinated ducks challenged with 5 x 10(8) DHBV genomes had an average of 31.5% and 9.2% of DHBV-positive hepatocytes on day 4 p.c. respectively and only 4 of the 18 vaccinated ducks were protected against chronic infection. There was no statistically significant difference in the efficacy of the DHBV pre-S/S or S DNA vaccines. In conclusion, vaccination of young ducks with DNA vaccines expressing the DHBV pre-S/S and S proteins induced rapid immune responses that reduced the extent of initial DHBV infection in the liver and prevented the development of chronic infection in a virus dose-dependent manner.
机译:我们测试了表达鸭乙型肝炎病毒(DHBV)的表面(pre-S / S)和表面(S)蛋白的DNA疫苗在改变14天大的鸭子感染结果中的功效。在两个实验中,分别在第4天和第14天分别用表达DHBV pre-S / S或S蛋白或对照质粒载体pcDNA1.1Amp的Pekin Aylesbury鸭子疫苗接种。然后在第14天的年龄对所有鸭子静脉注射5 x 10(7)或5 x 10(8)DHBV基因组。使用攻击后第4天收集的肝活检组织评估初始DHBV感染的水平(p.c.),然后对DHBV表面抗原进行免疫染色,以确定感染的肝细胞的百分比。在接种后第4天,用5 x 10(7)和5 x 10(8)DHBV基因组攻击的所有接种疫苗的鸭子平均分别具有DHBV阳性肝细胞的3.21%和20.1%。 16只鸭子中有16只出现了慢性DHBV感染。相反,用5 x 10(7)DHBV基因组攻击的前S / S和S疫苗免疫鸭子在初次第4天时的初始感染水平降低,平均DHBV阳性肝细胞为1.38%和1.93%。分别保护了18只鸭子中的10只免受慢性感染。在接种后第4天,用5 x 10(8)DHBV基因组攻击的pre-S / S和S DNA疫苗免疫鸭子平均拥有31.5%和9.2%的DHBV阳性肝细胞。分别地,在18只疫苗接种的鸭子中只有4只受到保护,免受慢性感染。 DHBV pre-S / S或S DNA疫苗的功效在统计学上没有显着差异。总之,用表达DHBV pre-S / S和S蛋白的DNA疫苗对幼鸭进行疫苗接种可引起快速的免疫反应,从而减少了肝脏中最初DHBV感染的程度,并以病毒剂量依赖性的方式阻止了慢性感染的发展。 。

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