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自分层聚氨酯-聚脲纳米颗粒中的纳米包封布地奈德在诱导人耐受性树突状细胞方面非常有效。

Nanoencapsulated budesonide in self-stratified polyurethane-polyurea nanoparticles is highly effective in inducing human tolerogenic dendritic cells.

作者信息

Flórez-Grau Georgina, Rocas Pau, Cabezón Raquel, España Carolina, Panés Julián, Rocas Josep, Albericio Fernando, Benítez-Ribas Daniel

机构信息

Institut d'Investigacions Biomèdiques August Pi i Sunyer (IDIBAPS), Barcelona, Spain.

Institute for Research in Biomedicine (IRB Barcelona), The Barcelona Institute of Science and Technology, Barcelona, Spain.

出版信息

Int J Pharm. 2016 Sep 25;511(2):785-93. doi: 10.1016/j.ijpharm.2016.07.056. Epub 2016 Jul 28.

Abstract

The design of innovative strategies to selectively target cells, such antigen-presenting cells and dendritic cells, in vivo to induce immune tolerance is gaining interest and relevance for the treatment of immune-mediated diseases. A novel loaded-nanosystem strategy to generate tolerogenic dendritic cells (tol-DCs) was evaluated. Hence budesonide (BDS) was encapsulated in multiwalled polyurethane-polyurea nanoparticles (PUUa NPs-BDS) based on self-stratified polymers by hydrophobic interactions at the oil-water interface. DCs treated with encapsulated BDS presented a prominent downregulation of costimulatory molecules (CD80, CD83 and MHCII) and upregulation of inhibitory receptors. Moreover, DCs treated with these PUUa NPs-BDS also secreted large amounts of IL-10, a crucial anti-inflammatory cytokine to induce tolerance, and inhibited T lymphocyte activation in a specific manner compared to those cells generated with free BDS. These results demonstrate that PUUa NPs-BDS are a highly specific and efficient system through which to induce DCs with a tolerogenic profile. Given the capacity of PUUa NPs-BDS, this delivery system has a clear advantage for translation to in vivo studies.

摘要

设计创新策略以在体内选择性靶向细胞(如抗原呈递细胞和树突状细胞)来诱导免疫耐受,对于免疫介导疾病的治疗正变得越来越受关注且具有重要意义。评估了一种用于生成耐受性树突状细胞(tol-DC)的新型负载纳米系统策略。因此,布地奈德(BDS)通过油水界面的疏水相互作用被封装在基于自分层聚合物的多壁聚氨酯-聚脲纳米颗粒(PUUa NPs-BDS)中。用封装的BDS处理的树突状细胞共刺激分子(CD80、CD83和MHCII)显著下调,抑制性受体上调。此外,与用游离BDS产生的细胞相比,用这些PUUa NPs-BDS处理的树突状细胞还分泌大量IL-10(一种诱导耐受的关键抗炎细胞因子),并以特定方式抑制T淋巴细胞活化。这些结果表明,PUUa NPs-BDS是一种高度特异性和高效的系统,可通过该系统诱导具有耐受性特征的树突状细胞。鉴于PUUa NPs-BDS的能力,这种递送系统在转化为体内研究方面具有明显优势。

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