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Recent advances in antibody-inducing poxviral and adenoviral vectored vaccine delivery platforms for difficult disease targets

机译:用于困难疾病靶标的抗体诱导型痘病毒和腺病毒载体疫苗输送平台的最新进展

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摘要

Viral vectored vaccine delivery platforms have traditionally been used for the induction of cellular rather than humoral immunity. However, in recent years, recombinant adenoviral and poxviral vectored vaccines have been optimized to induce B-cell responses, resulting in the demonstration of high-titer antibody responses in a wide variety of animal species. These approaches have now been translated, confirming the induction of substantial levels of antigen-specific IgG in a series of Phase I human clinical trials targeting HIV-1 and Plasmodium falciparum malaria. To further improve the induction of antibodies, mixed-modality regimens based on recombinant viral and protein/adjuvant vaccines are now being assessed. However, limited data exist about the underlying mechanisms mediating the induction of B-cell responses by these subunit vaccines and their ability to influence the qualitative aspects of vaccine-induced B-cell populations and immunoglobulin. Future studies in this area are needed to guide the rational design of antibody-inducing subunit vaccine strategies.
机译:病毒载体疫苗递送平台传统上已用于诱导细胞而非体液免疫。然而,近年来,重组腺病毒和痘病毒载体疫苗已被优化以诱导B细胞反应,从而在多种动物物种中证明了高滴度抗体反应。现在已经翻译了这些方法,证实了在针对HIV-1和恶性疟原虫疟疾的一系列I期人类临床试验中诱导了大量抗原特异性IgG的产生。为了进一步改善抗体的诱导,目前正在评估基于重组病毒和蛋白质/佐剂疫苗的混合模式方案。但是,关于介导这些亚基疫苗诱导B细胞应答的潜在机制及其影响疫苗诱导B细胞群体和免疫球蛋白定性方面的能力的数据尚有限。需要在该领域中进行进一步的研究以指导抗体诱导亚单位疫苗策略的合理设计。

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