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Enhancing the Stability and Potency of the Adjuvant Poly(I:C) through Nanoparticle Encapsulation

机译:通过纳米粒子包封增强佐剂聚(I:C)的稳定性和效力

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I synthesized, characterized, and screened a combinatorial library of poly(I:C)-loaded PBAE NPs. Many polymer NPs enhanced the potency of poly(I:C) in vivo and NP 5 led to an unprecedented 13X increase in activation and did not cause systemic toxicity. I selected promising NPs and tested their ability to enhance the immune response to ova antigen in vivo. I found that NP 5 greatly enhanced the humoral immune response (increased antibody concentration and affinity) to ova. Additionally, vaccination with NPs of varying polymer chemistry altered the IgG1:IgG2c ratio, suggesting we can tune polymer chemistry to skew the immune response (Th1 vs. Th2).
机译:I合成,特征和筛选聚(I:C)的组合文库 - 加载的PBAE NPS。许多聚合物NPS增强了聚(I:C)在体内(I:C)的效力,NP 5导致了前所未有的13倍的活化增加,并且没有引起全身毒性。我选择了有前途的NPS,并测试了它们在体内增强对ova抗原的免疫应答的能力。我发现NP 5大大提高了对胚芽的体液免疫反应(增加抗体浓度和亲和力)。另外,具有不同聚合物化学的NPS的疫苗接种改变了IgG1:IgG2C比,表明我们可以调节聚合物化学来倾斜免疫应答(Th1与Th2)。

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