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聚酸酐微球通过化学依赖方式吸附血清蛋白,从而影响树突状细胞的摄取和激活。

Chemistry-dependent adsorption of serum proteins onto polyanhydride microparticles differentially influences dendritic cell uptake and activation.

机构信息

Department of Chemical and Biological Engineering, Iowa State University, Ames, IA 50011, USA.

出版信息

Acta Biomater. 2012 Oct;8(10):3618-28. doi: 10.1016/j.actbio.2012.06.001. Epub 2012 Jun 8.

DOI:10.1016/j.actbio.2012.06.001
PMID:22684115
Abstract

The delivery of antigen-loaded microparticles to dendritic cells (DCs) may benefit from surface optimization of the microparticles themselves, thereby exploiting the material properties and introducing signals that mimic pathogens. Following in vivo administration microparticle surface characteristics are likely to be significantly modified as proteins are quickly adsorbed onto their surface. In this work we describe the chemistry-dependent serum protein adsorption patterns on polyanhydride particles and the implications for their molecular interactions with DCs. The enhanced expression of MHC II and CD40 on DCs after incubation with amphiphilic polyanhydride particles, and the increased secretion of IL-6, TNF-α, and IL-12p40 by hydrophobic polyanhydride particles exemplified the chemistry-dependent activation of DCs by sham-coated particles. The presence of proteins such as complement component 3 and IgG further enhanced the adjuvant properties of these vaccine carriers by inducing DC maturation (i.e. increased cell surface molecule expression and cytokine secretion) in a chemistry-dependent manner. Utilizing DCs derived from complement receptor 3-deficient mice (CR3(-/-) mice) identified a requirement for CR3 in the internalization of both sham- and serum-coated particles. These studies provide valuable insights into the rational design of targeted vaccine platforms aimed at inducing robust immune responses and improving vaccine efficacy.

摘要

将负载抗原的微粒递送至树突状细胞 (DC) 中可能受益于微粒本身的表面优化,从而利用材料特性并引入模拟病原体的信号。在体内给药后,由于蛋白质迅速吸附在微粒表面上,因此微粒表面特性可能会发生明显改变。在这项工作中,我们描述了聚酸酐颗粒上依赖化学性质的血清蛋白吸附模式及其与 DC 分子相互作用的意义。亲脂性聚酸酐颗粒孵育后 DC 表面 MHC II 和 CD40 的表达增强,以及疏水性聚酸酐颗粒中 IL-6、TNF-α 和 IL-12p40 的分泌增加,都说明了 sham 涂层颗粒可依赖化学性质激活 DC。补体成分 3 和 IgG 等蛋白质的存在通过以化学依赖的方式诱导 DC 成熟(即增加细胞表面分子表达和细胞因子分泌)进一步增强了这些疫苗载体的佐剂特性。利用补体受体 3 缺陷型小鼠 (CR3(-/-) 小鼠) 的 DC 证明了 CR3 对 sham 和血清包被颗粒内化的必要性。这些研究为旨在诱导强大免疫反应和提高疫苗功效的靶向疫苗平台的合理设计提供了有价值的见解。

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