编码非结构蛋白1 -2型登革热病毒重组DNA疫苗在Balb/c小鼠中的免疫原性

Fithriyah Sjatha, Elitha Sundari Pulungan, T. M. Sudiro
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摘要

登革出血热(DHF)是由登革热病毒(DENV)引起的一种传染病,在世界热带和亚热带地区广泛传播。DENV是一种基因组大小为±11kb的单正链RNA病毒,编码3种结构蛋白、7种非结构蛋白和2个非翻译区(UTR)。DENV的非结构蛋白-1 (NS1)在登革热发病机制中具有重要作用,有望开发成登革热疫苗。近年来,DNA免疫的新疫苗途径为构建安全、稳定、免疫原性强的疫苗平台提供了新的视角。此前,我们已经成功构建了编码DENV2 NS1蛋白的DNA疫苗(pUNS1),该疫苗在哺乳动物细胞系中表达重组NS1蛋白。因此,本研究将通过小鼠免疫进一步分析pUNS1诱导体液免疫应答的能力。16只4周龄BALB/c小鼠,每隔2周注射100µg pUNS1或pUMVC4a免疫3次。仅在免疫前采血,最后一次免疫后2周终止。用室内ELISA检测小鼠血清中DENV-2抗体滴度。重组pUNS1免疫组小鼠抗登革热NS1 IgG滴度比pUMVC4a组高5倍。这一结果提示pUNS1能够在体内诱导针对NS1 DENV-2的体液免疫应答。重组pUNS1可诱导小鼠体液免疫应答。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Immunogenicity of Recombinant DNA Vaccine Encoding Non-Structural Protein-1 Dengue Virus Serotype-2 in Balb/c Mice
Dengue Hemorrhagic Fever (DHF) is an infectious disease caused by the dengue virus (DENV) which spread widely in tropical and subtropical regions of the world. DENV is a single-positive strand RNA virus with a genome size of ± 11kb which encodes three structural proteins, seven non-structural proteins, and two untranslated regions (UTR). The non-structural protein-1 (NS1) of DENV is known to have important role in dengue pathogenesis also promising to be developed as dengue vaccine. Lately, novel vaccine approach by DNA immunization have given new perspective for a safe, stable, and immunogenic vaccine platform. Previously, we had successfully constructed DNA vaccine encoding NS1 protein of DENV2 (pUNS1) which expressed recombinant NS1 protein in mammalian cells line. Thus, in this current study the ability of pUNS1 to induce humoral immune response will be further analyzed by in mice immunization. Sixteen BALB/c mice aged of 4 weeks were immunized 3 times with 100 µg of pUNS1 or pUMVC4a on 2 weeks interval. Blood sampling was carried out just before immunization and termination was done 2 weeks after last immunization. Antibodies titer from individual mice sera against DENV-2 were measured with in-house ELISA. Anti-dengue NS1 IgG titer from mice group immunized with recombinant pUNS1 Showed ELISA absorbances five times higher than pUMVC4a group. This result suggested the ability of pUNS1 to induce humoral immune response against NS1 DENV-2 in-vivo. Recombinant pUNS1 can induce humoral immune response in mice.
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