针对Peyer’s补丁M细胞的粘膜疫苗。

Behring Institute Mitteilungen Pub Date : 1997-02-01
A Frey, M R Neutra
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引用次数: 0

摘要

抗原和病原体的经上皮运输是诱导粘膜免疫反应的第一步。在肠道中,抗原通过上皮屏障传递到淋巴组织是由M细胞完成的,M细胞是一种特殊的上皮细胞类型,只发生在淋巴滤泡相关上皮中。M细胞选择性和高效地转运抗原被认为是有效的粘膜疫苗的基本要求。因此,目前正在开发颗粒抗原制剂,以利用M细胞内吞颗粒的能力。基于病原体利用M细胞作为侵入人体的途径,使用基因工程、脊髓灰质炎病毒和沙门氏菌等病原体的减毒菌株设计了粘膜活疫苗。在另一种方法,抗原偶联或封装在颗粒合成载体。为了增强这种不存活载体的结合和摄取,配体被附着,将疫苗颗粒引导到M细胞表面的受体上。
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Targeting of mucosal vaccines to Peyer's patch M cells.

Transepithelial transport of antigens and pathogens is the first step in the induction of a mucosal immune response. In the intestine, the delivery of antigens across the epithelial barrier to the underlying lymphoid tissue is accomplished by M cells, a specialized epithelial cell type that occurs only in the lymphoid follicle-associated epithelium. Selective and efficient transport of antigen by M cells is considered an essential requirement for effective mucosal vaccines. Therefore, particulate antigen formulations are currently being developed to take advantage of the capacity of M cells to endocytose particles. Based on pathogens that exploit the M cell as an invasion route into the body, live mucosal vaccines have been designed using genetically-engineered, attenuated strains of pathogens such as poliovirus and Salmonella. In an alternative approach, antigens are coupled to or encapsulated in particulate synthetic carriers. To enhance binding and uptake of such nonviable vectors, ligands are being attached which direct the vaccine particle to receptors on the M cell surface.

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