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模仿微生物策略设计用于口服免疫的可渗透黏液纳米颗粒。

Mimicking microbial strategies for the design of mucus-permeating nanoparticles for oral immunization.

作者信息

Gamazo Carlos, Martín-Arbella Nekane, Brotons Ana, Camacho Ana I, Irache J M

机构信息

Department of Microbiology, University of Navarra, Pamplona, Spain.

Department of Pharmacy and Pharmaceutical Technology, University of Navarra, Pamplona, Spain.

出版信息

Eur J Pharm Biopharm. 2015 Oct;96:454-63. doi: 10.1016/j.ejpb.2015.01.010. Epub 2015 Jan 20.

Abstract

Dealing with mucosal delivery systems means dealing with mucus. The name mucosa comes from mucus, a dense fluid enriched in glycoproteins, such as mucin, which main function is to protect the delicate mucosal epithelium. Mucus provides a barrier against physiological chemical and physical aggressors (i.e., host secreted digestive products such as bile acids and enzymes, food particles) but also against the potentially noxious microbiota and their products. Intestinal mucosa covers 400m(2) in the human host, and, as a consequence, is the major portal of entry of the majority of known pathogens. But, in turn, some microorganisms have evolved many different approaches to circumvent this barrier, a direct consequence of natural co-evolution. The understanding of these mechanisms (known as virulence factors) used to interact and/or disrupt mucosal barriers should instruct us to a rational design of nanoparticulate delivery systems intended for oral vaccination and immunotherapy. This review deals with this mimetic approach to obtain nanocarriers capable to reach the epithelial cells after oral delivery and, in parallel, induce strong and long-lasting immune and protective responses.

摘要

处理黏膜给药系统意味着要应对黏液。黏膜这个名称源自黏液,黏液是一种富含糖蛋白(如黏蛋白)的浓稠液体,其主要功能是保护脆弱的黏膜上皮。黏液可抵御生理化学和物理侵害者(即宿主分泌的消化产物,如胆汁酸和酶、食物颗粒),还能抵御潜在有害的微生物群及其产物。人类宿主的肠道黏膜面积达400平方米,因此是大多数已知病原体的主要入侵门户。但是,反过来,一些微生物已经进化出许多不同的方法来规避这一屏障,这是自然共同进化的直接结果。了解这些用于相互作用和/或破坏黏膜屏障的机制(称为毒力因子),应该能指导我们合理设计用于口服疫苗接种和免疫治疗的纳米颗粒给药系统。本综述探讨了这种模拟方法,以获得能够在口服给药后到达上皮细胞并同时诱导强烈而持久的免疫和保护反应的纳米载体。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7252/7126451/ff52446d26a7/fx1_lrg.jpg

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