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首页> 外文期刊>Journal of Controlled Release: Official Journal of the Controlled Release Society >Investigation of tunable acetalated dextran microparticle platform to optimize M2e-based influenza vaccine efficacy
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Investigation of tunable acetalated dextran microparticle platform to optimize M2e-based influenza vaccine efficacy

机译:调节乙型葡聚糖微粒平台优化M2E型流感疫苗疗效的调查

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Influenza places a significant health and economic burden on society. Efficacy of seasonal influenza vaccines can be suboptimal due to poor matching between vaccine and circulating viral strains. An influenza vaccine that is broadly protective against multiple virus strains would significantly improve vaccine efficacy. The highly conserved ectodomain of matrix protein 2 (M2e) and 3'3' cyclic GMP-AMP (cGAMP) were selected as the antigen and adjuvant, respectively, to develop the basis for a potential universal influenza vaccine. The magnitude and kinetics of adaptive immune responses can have great impact on vaccine efficacy. M2e and cGAMP were therefore formulated within acetalated dextran (Ace-DEX) microparticles (MPs) of varying degradation profiles to examine the effect of differential vaccine delivery on humoral, cellular, and protective immunity. All Ace-DEX MP vaccines containing M2e and cGAMP elicited potent humoral and cellular responses in vivo and offered substantial protection against a lethal influenza challenge, suggesting significant vaccine efficacy. Serum antibodies from Ace-DEX MP vaccinated mice also demonstrated cross reactivity against M2e sequences of various viral strains, which indicates the potential for broadly protective immunity. Of all the formulations tested, the slowest-degrading M2e or cGAMP MPs elicited the greatest antibody production, cellular response, and protection against a viral challenge. This indicated the importance of flexible control over antigen and adjuvant delivery. Overall, robust immune responses, cross reactivity against multiple viral strains, and tunable delivery profiles make the Ace-DEX MP platform a powerful subunit vaccine delivery system.
机译:流感对社会产生重大的健康和经济负担。由于疫苗和循环病毒菌株之间的匹配差,季节性流感疫苗的疗效可能是次优。广泛保护多种病毒菌株的流感疫苗会显着提高疫苗疗效。选择基质蛋白2(M2E)和3'3'环状GMP-AMP(CGAMP)的高度保守的外构造植物分别作为抗原和佐剂,以开发潜在的通用流感疫苗的基础。适应性免疫应答的幅度和动力学对疫苗疗效产生很大影响。因此,将M2E和CGAMP配制在不同劣化型材的乙酰甲醛(ACE-DEX)微粒(MPS)中,以检查差分疫苗输送对体液,细胞和保护性免疫的影响。含有M2E和CGAMP的所有ACE-DEX MP疫苗引发了体内有效的体液和细胞反应,并对致命性流感攻击提供了重大保护,表明显着的疫苗疗效。来自ACE-DEX MP接种疫苗小鼠的血清抗体也明确了针对各种病毒菌株的M2E序列的交叉反应性,这表明了广泛保护性免疫的可能性。在所有测试的配方中,最缓慢的降解的M2E或CGAMP MPS引发了最大的抗体生产,细胞反应和免受病毒攻击的保护。这表明灵活控制抗原和佐剂交付的重要性。总体而鲁棒的免疫应答,对多种病毒菌株的交叉反应性,以及可调谐的递送型材使ACE-DEX MP平台成为强大的亚基疫苗输送系统。

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