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Enhancement of Antibodies to the Human Immunodeficiency Virus Type 1 Envelope by Using the Molecular Adjuvant C3d

机译:通过使用分子佐剂C3d增强针对人类免疫缺陷病毒1型信封的抗体

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摘要

DNA vaccines expressing the envelope (Env) protein of the human immunodeficiency virus have been relatively ineffective at generating high-titer, long-lasting, neutralizing antibodies in a variety of animal models. In this study, the murine and human homologues of the complement component, C3d, were used in a DNA vaccine to enhance the titers of antibody to Env. Initially, plasmids expressing a secreted form of Env (sgp120) fused to one, two, or three copies of the murine homologue of C3d (mC3d) were constructed. Mice were inoculated with four vaccinations of DNA or two DNA vaccinations, followed by two boosts of affinity-purified gp120 protein. Analyses of titers demonstrated that multiple copies of mC3d coupled to sgp120 induced long-lasting, high-titer anti-Env antibody. Priming mice with sgp120-mC3d-DNA, followed by inoculation of purified gp120 protein, elicited the strongest antibody titers; however, the avidity maturation of the antibody was accelerated in the mice inoculated with sgp120-mC3d3-DNA. In addition, DNAs expressing sgp120 fused to three copies of the human homologue of C3d (hC3d3) efficiently enhanced the anti-Env antibody in rabbits. Lastly, antisera from both mice and rabbits vaccinated with DNA expressing sgp120-C3d3 elicited higher titers of neutralizing antibody than did nonfused forms of Env. These results indicate that C3d, conjugated to sgp120, enhances the antibody responses to Env compared to non-C3d fused forms of Env, and this approach may be one way to overcome the poor ability of DNA vaccines to generate antibodies to Env.
机译:在多种动物模型中,表达人类免疫缺陷病毒包膜(Env)蛋白的DNA疫苗在产生高滴度,长效,中和抗体方面相对无效。在这项研究中,补体成分C3d的鼠和人同源物被用于DNA疫苗中,以增强针对Env的抗体的效价。最初,构建了表达分泌形式的Env(sgp120)融合到C3d(mC3d)鼠同源物中的一个,两个或三个副本的质粒。给小鼠接种四次DNA疫苗或两次DNA疫苗,然后两次免疫亲和纯化的gp120蛋白。滴度分析表明,与sgp120偶联的多拷贝mC3d诱导了持久的高滴度抗Env抗体。用sgp120-mC3d-DNA引发小鼠,然后接种纯化的gp120蛋白,可产生最强的抗体滴度。但是,在接种sgp120-mC3d3-DNA的小鼠中,抗体的亲和力成熟得以加速。此外,与三份C3d人类同源物(hC3d3)融合的表达sgp120的DNA可有效增强兔的抗Env抗体。最后,接种了表达sgp120-C3d3的DNA的小鼠和兔子的抗血清引起的中和抗体的滴度要高于非融合形式的Env。这些结果表明,与非C3d融合形式的Env相比,与sgp120缀合的C3d增强了对Env的抗体反应,这种方法可能是克服DNA疫苗产生针对Env的抗体能力较弱的一种方法。

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