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A Trifunctional Dextran-Based Nanovaccine Targets and Activates Murine Dendritic Cells and Induces Potent Cellular and Humoral Immune Responses In Vivo

机译:基于三功能葡聚糖的纳米疫苗靶向并激活小鼠树突状细胞并诱导体内强效的细胞和体液免疫反应。

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摘要

Dendritic cells (DCs) constitute an attractive target for specific delivery of nanovaccines for immunotherapeutic applications. Here we tested nano-sized dextran (DEX) particles to serve as a DC-addressing nanocarrier platform. Non-functionalized DEX particles had no immunomodulatory effect on bone marrow (BM)-derived murine DCs in vitro. However, when adsorbed with ovalbumine (OVA), DEX particles were efficiently engulfed by BM-DCs in a mannose receptor-dependent manner. A DEX-based nanovaccine containing OVA and lipopolysaccharide (LPS) as a DC stimulus induced strong OVA peptide-specific CD4+ and CD8+ T cell proliferation both in vitro and upon systemic application in mice, as well as a robust OVA-specific humoral immune response (IgG1>IgG2a) in vivo. Accordingly, this nanovaccine also raised both a more pronounced delayed-type hypersensitivity response and a stronger induction of cytotoxic CD8+ T cells than obtained upon administration of OVA and LPS in soluble form. Therefore, DEX-based nanoparticles constitute a potent, versatile and easy to prepare nanovaccine platform for immunotherapeutic approaches.
机译:树突状细胞(DC)构成了纳米疫苗特异性递送用于免疫治疗应用的有吸引力的靶标。在这里,我们测试了纳米级右旋糖酐(DEX)颗粒作为DC寻址纳米载体平台。非功能化的DEX颗粒对骨髓(BM)衍生的鼠DC在体外没有免疫调节作用。但是,当被卵清蛋白(OVA)吸附时,DEX颗粒被甘露糖受体依赖性的BM-DC有效地吞噬。含有OVA和脂多糖(LPS)作为DC刺激的基于DEX的纳米疫苗可在体外和全身性诱导强OVA肽特异性CD4 + 和CD8 + T细胞增殖在小鼠中的应用,以及体内强大的OVA特异性体液免疫应答(IgG1> IgG2a)。因此,与以可溶形式施用OVA和LPS所获得的相比,这种纳米疫苗还引起了更明显的延迟型超敏反应和对细胞毒性CD8 + T细胞的更强诱导。因此,基于DEX的纳米颗粒构成了有效,多功能且易于制备的用于免疫治疗方法的纳米疫苗平台。

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