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多糖纳米胶囊中病毒蛋白和 TLR7 激动剂的共递送:一种无针疫苗接种策略。

Co-delivery of viral proteins and a TLR7 agonist from polysaccharide nanocapsules: a needle-free vaccination strategy.

机构信息

Center for Research in Molecular Medicine and Chronic Diseases (CIMUS), University of Santiago de Compostela, 15706 Campus Vida, Santiago de Compostela, Spain; Department of Pharmacy and Pharmaceutical Technology, School of Pharmacy, University of Santiago de Compostela, 15705 Campus Vida, Santiago de Compostela, Spain.

出版信息

J Control Release. 2013 Dec 28;172(3):773-81. doi: 10.1016/j.jconrel.2013.09.012. Epub 2013 Sep 25.

DOI:10.1016/j.jconrel.2013.09.012
PMID:24076340
Abstract

Here we report a new nanotechnology-based nasal vaccination concept intended to elicit both, specific humoral and cellular immune responses. The concept relies on the use of a multifunctional antigen nanocarrier consisting of a hydrophobic nanocore, which can allocate lipophilic immunostimulants, and a polymeric corona made of chitosan (CS), intended to associate antigens and facilitate their transport across the nasal mucosa. The Toll-like receptor 7 (TLR7) agonist, imiquimod, and the recombinant hepatitis B surface antigen (HB), were selected as model molecules for the validation of the concept. The multifunctional nanocarriers had a nanometric size (around 200 nm), a high positive zeta potential (+45 mV) and a high antigen association efficiency (70%). They also exhibited the ability to enter macrophages in vitro and to effectively deliver the associated imiquimod intracellularly, as noted by the secretion of pro-inflammatory cytokines (i.e. IL-6 and TNF-α). However, the nanocarriers did not induce the in vitro activation of the complement cascade. Finally, the positive effect of the co-delivery of HB and imiquimod from the nanocapsules was evidenced upon intranasal administration to mice. The nanocapsules containing imiquimod elicited a protective immune response characterized by increasing IgG levels over time and specific immunological memory. Additionally, the levels of serum IgG subclasses (IgG1 and IgG2a) indicated a balanced cellular/humoral response, thus suggesting the capacity of the nanocapsules to modulate the systemic immune response upon nasal vaccination.

摘要

在这里,我们报告了一种新的基于纳米技术的鼻腔免疫接种概念,旨在引发特异性体液和细胞免疫反应。该概念依赖于使用一种多功能抗原纳米载体,该载体由疏水纳米核组成,可分配亲脂性免疫刺激剂,以及由壳聚糖(CS)制成的聚合物冠,旨在结合抗原并促进它们穿过鼻黏膜的运输。Toll 样受体 7(TLR7)激动剂咪喹莫特和重组乙型肝炎表面抗原(HB)被选为验证该概念的模型分子。多功能纳米载体具有纳米级尺寸(约 200nm)、高正 zeta 电位(+45mV)和高抗原结合效率(70%)。它们还表现出能够进入体外巨噬细胞并有效地将相关咪喹莫特递送到细胞内的能力,这可以通过分泌促炎细胞因子(即 IL-6 和 TNF-α)来证明。然而,纳米载体并没有诱导体外补体级联的激活。最后,在向小鼠鼻腔内给药时,证明了从纳米胶囊中共同递送 HB 和咪喹莫特的积极效果。含有咪喹莫特的纳米胶囊引发了保护性免疫反应,表现为 IgG 水平随时间的增加和特异性免疫记忆。此外,血清 IgG 亚类(IgG1 和 IgG2a)的水平表明了细胞/体液反应的平衡,因此表明纳米胶囊有能力在鼻腔免疫接种时调节全身免疫反应。

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