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人肠道上皮细胞高度极化的HLA-II类抗原加工与呈递

Highly polarized HLA class II antigen processing and presentation by human intestinal epithelial cells.

作者信息

Hershberg R M, Cho D H, Youakim A, Bradley M B, Lee J S, Framson P E, Nepom G T

机构信息

Virginia Mason Research Center, Seattle, Washington 98101, USA.

出版信息

J Clin Invest. 1998 Aug 15;102(4):792-803. doi: 10.1172/JCI3201.

Abstract

The high concentration of foreign antigen in the lumen of the gastrointestinal tract is separated from the underlying lymphocytes by a single cell layer of polarized epithelium. Intestinal epithelial cells can express HLA class II antigens and may function as antigen-presenting cells to CD4(+) T cells within the intestinal mucosa. Using tetanus toxoid specific and HLA-DR-restricted T lymphocytes, we show that polarized intestinal epithelial cells directed to express HLA-DR molecules are able to initiate class II processing only after internalization of antigen from their apical surface. Coexpression of the class II transactivator CIITA in these cells, which stimulates highly efficient class II processing without the characteristic decline in barrier function seen in polarized monolayers treated with the proinflammatory cytokine gamma-IFN, facilitates antigen processing from the basolateral surface. In both cases, peptide presentation to T cells via class II molecules was restricted to the basolateral surface. These data indicate a highly polarized functional architecture for antigen processing and presentation by intestinal epithelial cells, and suggest that the functional outcome of antigen processing by the intestinal epithelium is both dependent on the cellular surface at which the foreign antigen is internalized and by the underlying degree of mucosal inflammation.

摘要

胃肠道管腔内的高浓度外来抗原通过一层极化上皮细胞与下方的淋巴细胞分隔开来。肠上皮细胞可表达II类HLA抗原,并可能作为肠黏膜内CD4(+) T细胞的抗原呈递细胞发挥作用。利用破伤风类毒素特异性且受HLA-DR限制的T淋巴细胞,我们发现,定向表达HLA-DR分子的极化肠上皮细胞只有在从其顶端表面内化抗原后才能启动II类加工过程。在这些细胞中共同表达II类反式激活因子CIITA,可刺激高效的II类加工过程,且不会出现用促炎细胞因子γ-干扰素处理的极化单层细胞中所见的屏障功能特征性下降,这有助于从基底外侧表面进行抗原加工。在这两种情况下,通过II类分子向T细胞呈递肽均局限于基底外侧表面。这些数据表明肠上皮细胞进行抗原加工和呈递具有高度极化的功能结构,并提示肠上皮进行抗原加工的功能结果既取决于内化外来抗原的细胞表面,也取决于下方黏膜炎症的程度。

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