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壳聚糖纳米载体在黏膜免疫疫苗学中的效率

Efficiency of Chitosan Nanocarriers in Vaccinology for Mucosal Immunization.

作者信息

Gaglio Salvatore Calogero, Perduca Massimiliano, Zipeto Donato, Bardi Giuseppe

机构信息

Department of Biotechnology, University of Verona, Cà Vignal 1, Strada Le Grazie 15, 37134 Verona, Italy.

Department of Neurosciences, Biomedicine and Movement Sciences, University of Verona, Strada Le Grazie 8, 37134 Verona, Italy.

出版信息

Vaccines (Basel). 2023 Aug 6;11(8):1333. doi: 10.3390/vaccines11081333.

Abstract

The mucosal barrier constitutes a huge surface area, close to 40 m in humans, located mostly in the respiratory, gastrointestinal and urogenital tracts and ocular cavities. It plays a crucial role in tissue interactions with the microbiome, dietary antigens and other environmental materials. Effective vaccinations to achieve highly protective mucosal immunity are evolving strategies to counteract several serious diseases including tuberculosis, diphtheria, influenzae B, severe acute respiratory syndrome, Human Papilloma Virus infection and Acquired Immune Deficiency Syndrome. Interestingly, one of the reasons behind the rapid spread of severe acute respiratory syndrome coronavirus 2 variants has been the weakness of local immunization at the level of the respiratory mucosa. Mucosal vaccines can outperform parenteral vaccination as they specifically elicit protective mucosal immune responses blocking infection and transmission. In this scenario, chitosan-based nanovaccines are promising adjuvants-carrier systems that rely on the ability of chitosan to cross tight junctions and enhance particle uptake due to chitosan-specific mucoadhesive properties. Indeed, chitosan not only improves the adhesion of antigens to the mucosa promoting their absorption but also shows intrinsic immunostimulant abilities. Furthermore, by finely tuning the colloidal properties of chitosan, it can provide sustained antigen release to strongly activate the humoral defense. In the present review, we agnostically discuss the potential reasons why chitosan-based vaccine carriers, that efficiently elicit strong immune responses in experimental setups and in some pre-clinical/clinical studies, are still poorly considered for therapeutic formulations.

摘要

黏膜屏障构成了一个巨大的表面积,在人类中接近40平方米,主要位于呼吸道、胃肠道、泌尿生殖道和眼腔。它在组织与微生物群、饮食抗原和其他环境物质的相互作用中起着关键作用。实现高度保护性黏膜免疫的有效疫苗接种是应对包括结核病、白喉、B型流感嗜血杆菌、严重急性呼吸综合征、人乳头瘤病毒感染和获得性免疫缺陷综合征在内的几种严重疾病的不断发展的策略。有趣的是,严重急性呼吸综合征冠状病毒2变体迅速传播的原因之一是呼吸道黏膜水平的局部免疫薄弱。黏膜疫苗可以优于注射疫苗,因为它们能特异性地引发保护性黏膜免疫反应,阻止感染和传播。在这种情况下,基于壳聚糖的纳米疫苗是有前景的佐剂-载体系统,这依赖于壳聚糖穿过紧密连接的能力以及由于壳聚糖特异性的黏膜黏附特性而增强颗粒摄取。事实上,壳聚糖不仅能改善抗原与黏膜的黏附,促进其吸收,还具有内在的免疫刺激能力。此外,通过精细调节壳聚糖的胶体性质,它可以实现抗原的持续释放,从而强烈激活体液防御。在本综述中,我们客观地讨论了基于壳聚糖的疫苗载体在实验设置以及一些临床前/临床研究中能有效引发强烈免疫反应,但在治疗制剂中仍未得到充分考虑的潜在原因。

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