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The impact of nanoparticle ligand density on dendritic-cell targeted vaccines.

机译:纳米粒子配体密度对树突状细胞靶向疫苗的影响。

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摘要

Dendritic-cell (DC) targeted antigen delivery systems hold promise for enhancing vaccine efficacy and delivery of therapeutics. However, it is not known how the number and density of targeting ligands on such systems may affect DC function and subsequent T cell response. We modified the surface of biodegradable nanoparticles loaded with antigen with different densities of the mAb to the DC lectin DEC-205 receptor and assessed changes in the cytokine response of DCs and T cells. DEC-205 targeted nanoparticles unexpectedly induced a differential cytokine response that depended on the density of ligands on the surface. Strikingly, nanoparticle surface density of DEC-205 mAb increased the amount of anti-inflammatory, IL-10, produced by DCs and T cells. Boosting mice with DEC-205 targeted OVA-nanoparticles after immunization with an antigen in CFA induced a similar pattern of IL-10 response. The correlation between DC production of IL-10 as a function of the density of anti-DEC-205 is shown to be due to cross-linking of the DEC-205 receptor. Cross-linking also increased DC expression of the scavenger receptor CD36, and blockade of CD36 largely abrogated the IL-10 response. Our studies highlight the importance of target ligand density in the design of vaccine delivery systems.
机译:树突状细胞(DC)靶向抗原递送系统有望增强疫苗效力和治疗剂的递送。但是,尚不知道这种系统上靶向配体的数量和密度如何影响DC功能和随后的T细胞反应。我们修饰了负载有抗原的生物可降解纳米颗粒的表面,该抗原具有不同密度的mAb对DC凝集素DEC-205受体,并评估了DC和T细胞的细胞因子反应的变化。 DEC-205靶向纳米颗粒出乎意料地诱导了不同的细胞因子反应,这取决于表面上配体的密度。令人惊讶的是,DEC-205 mAb的纳米颗粒表面密度增加了DC和T细胞产生的抗炎剂IL-10的数量。用CFA中的抗原免疫后,用DEC-205靶向的OVA-纳米颗粒加强小鼠的IL-10反应模式相似。显示IL-10的DC产生与抗DEC-205的密度之间的函数之间的相关性是由于DEC-205受体的交联。交联还增加了清道夫受体CD36的DC表达,并且CD36的阻断在很大程度上消除了IL-10应答。我们的研究突出了目标配体密度在疫苗输送系统设计中的重要性。

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