Antigen sampling by epithelial tissues: implication for vaccine design.

Behring Institute Mitteilungen Pub Date : 1997-02-01
J P Kraehenbuhl, S A Hopkins, S Kernéis, E Pringault
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Abstract

Mucosal surfaces of the respiratory, digestive and urogenital tracts are covered by a specialized epithelium which constitutes an efficient physical barrier against environmental pathogens. These surfaces differ greatly in their cellular organisation and in antigen sampling. In stratified epithelia, professional antigen-presenting cells, the dendritic cells or Langerhans cells, are intimately associated with the epithelial barrier and take up samples of foreign material from the external environment which they transport to local or distant organized lymphoid tissues. In simple epithelia highly specialised cells, the so-called M cells, sample foreign material and microorganisms and deliver them by transepithelial transport from the lumen to the underlying organized lymphoid tissue (MALT). The interaction of lymphocytes with the follicle-associated epithelium (FAE) is responsible for the loss of digestive functions and the acquisition of transepithelial transport activity. The three way interaction of epithelium, lymphoid cells, and microorganisms seen in the FAE which controls the formation of MALT provides a dramatic demonstration of the phenotypic plasticity of the intestinal epithelium and probably of all simple epithelia. We have shown that all mucosal surfaces, covered by stratified or simple epithelia are able to sample and transport live recombinant bacterial vaccines, which elicit systemic and local immune responses against the carrier and the foreign antigen. In gut and nasal-associated lymphoid tissue, Salmonella are taken up by dendritic cells which form a dense cellular network in the dome regions of MALT. Targeting bacterial vaccine candidates to dendritic or M cells is likely to facilitate their sampling by epithelial tissues and to contribute to strong mucosal and systemic immune responses.

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上皮组织抗原取样:疫苗设计的意义。
呼吸道、消化道和泌尿生殖道的粘膜表面覆盖着一层特殊的上皮,它构成了对抗环境病原体的有效物理屏障。这些表面在细胞组织和抗原取样上差别很大。在分层上皮中,专业抗原呈递细胞,树突状细胞或朗格汉斯细胞,与上皮屏障密切相关,并从外部环境中吸收外来物质样本,并将其运输到局部或远处有组织的淋巴组织。在简单上皮中,高度特化的细胞,即所谓的M细胞,采集外来物质和微生物,并通过上皮运输将它们从管腔运送到下层的有组织淋巴组织(MALT)。淋巴细胞与滤泡相关上皮(FAE)的相互作用导致了消化功能的丧失和上皮转运活性的获得。在FAE中,上皮、淋巴样细胞和微生物的三向相互作用控制着MALT的形成,这有力地证明了肠上皮和所有简单上皮的表型可塑性。我们已经证明,被分层上皮或单层上皮覆盖的所有粘膜表面都能够取样和运输活重组细菌疫苗,从而引发针对载体和外来抗原的全身和局部免疫反应。在肠道和鼻相关淋巴组织中,沙门氏菌被树突状细胞吸收,树突状细胞在MALT的圆顶区域形成密集的细胞网络。将细菌候选疫苗靶向树突状细胞或M细胞,可能有助于上皮组织对其进行取样,并有助于产生强烈的粘膜和全身免疫反应。
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