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表皮微穿孔增强经皮疫苗接种的效果。

Epidermal micro-perforation potentiates the efficacy of epicutaneous vaccination.

机构信息

DBV Technologies, Montrouge, France.

DBV Technologies, Montrouge, France.

出版信息

J Control Release. 2019 Mar 28;298:12-26. doi: 10.1016/j.jconrel.2019.02.004. Epub 2019 Feb 6.

DOI:10.1016/j.jconrel.2019.02.004
PMID:30738084
Abstract

The skin is an immune organ comprised of a large network of antigen-presenting cells such as dendritic cells, making it an attractive target for the development of new vaccines and immunotherapies. Recently, we developed a new innovative and non-invasive vaccination method without adjuvant based on epicutaneous vaccine patches on which antigen forms a dry deposit. Here we describe in mice a method for potentiating the efficacy of our epicutaneous vaccination approach using a minimally invasive and epidermis-limited skin preparation based on laser-induced micro-perforation. Our results showed that epidermal micro-perforation increased trans-epidermal water loss, resulting in an enhancement of antigen solubilization from the surface of the patch, and increased the quantity of antigen delivered to the epidermis. Importantly, this was not associated with an increase in systemic passage of the antigen. Skin micro-perforation slightly activated keratinocytes without inducing an excessive level of local inflammation. Moreover, epidermal micro-perforation improved antigen capture by epidermal dendritic cells and specifically increased the level of Langerhans cells activation. Finally, we observed that epidermal micro-perforation significantly increased the level of the specific antibody response induced by our epicutaneous Pertussis vaccine candidate containing non-adsorbed recombinant Pertussis Toxin and reduced the amount of antigen dose required. Overall, these data confirm the benefit of a minimal and controlled epidermal preparation for improving the effectiveness of an epicutaneous patch-based vaccine, without adversely affecting the safety of the method.

摘要

皮肤是一个由大量抗原呈递细胞(如树突状细胞)组成的免疫器官,使其成为开发新型疫苗和免疫疗法的有吸引力的目标。最近,我们开发了一种基于经皮疫苗贴剂的新型非侵入性疫苗接种方法,该方法无需佐剂,抗原在贴剂上形成干燥沉积物。在这里,我们在小鼠中描述了一种使用基于激光诱导微穿孔的微创和表皮限制皮肤制剂来增强我们经皮疫苗接种方法效果的方法。我们的结果表明,表皮微穿孔增加了经皮水分流失,导致贴剂表面的抗原溶解增强,并增加了递送至表皮的抗原量。重要的是,这与抗原的全身通透性增加无关。皮肤微穿孔轻微激活角质形成细胞,而不会引起过度的局部炎症。此外,表皮微穿孔改善了表皮树突状细胞对抗原的捕获,特别是增加了朗格汉斯细胞的激活水平。最后,我们观察到表皮微穿孔显著增加了我们含有未吸附重组百日咳毒素的经皮百日咳候选疫苗诱导的特异性抗体反应水平,并减少了所需抗原剂量。总的来说,这些数据证实了最小和可控的表皮制剂对于提高基于经皮贴剂疫苗的有效性的益处,而不会对该方法的安全性产生不利影响。

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