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树突状细胞获取抗原:肠道树突状细胞获取经口服给予的抗原,并能在体内启动初始T细胞。

Antigen acquisition by dendritic cells: intestinal dendritic cells acquire antigen administered orally and can prime naive T cells in vivo.

作者信息

Liu L M, MacPherson G G

机构信息

Sir William Dunn School of Pathology, University of Oxford, United Kingdom.

出版信息

J Exp Med. 1993 May 1;177(5):1299-307. doi: 10.1084/jem.177.5.1299.

Abstract

In the rat, mesenteric lymphadenectomy allows collection of dendritic cells (DC) derived from the small intestine after cannulation of the thoracic duct. We prepared rats this way and administered antigens by oral feeding or intraintestinal injection. DC enriched from the thoracic duct lymph collected over the first 24 h from these animals are able to stimulate sensitized T cells in vitro and to prime popliteal lymph node CD4+ T cells after footpad injection, while B and T cells from the same thoracic duct lymph are inert in priming. 500 or less DC pulsed in vitro with antigen can prime T cells in vivo, whereas 100 times more B cells or macrophages pulsed in vitro are quite inert. 1 mg of ovalbumin administered orally is sufficient to load DC for in vivo priming of T cells. Antigen could not be detected directly in DC but was present in macrophages in the lamina propria. Direct presentation of antigen by DC to T cells was demonstrated by injecting F1 recipients with parental DC and showing restriction of T cell sensitization to the major histocompatibility complex of the injected DC. Antigen-bearing DC do not induce a detectable primary antibody response but a small secondary antibody response can be detected after a boosting injection. These results show that acquisition of antigens by DC in the intestine is very similar to what occurs in vitro or in other tissues, suggesting that there may be no special difference in antigen handling at mucosal surfaces. One implication of these results is that hypotheses designed to explain oral tolerance must take into account the presence of immunostimulatory, antigen-bearing DC in animals that have received oral antigens.

摘要

在大鼠中,肠系膜淋巴结切除术可在胸导管插管后收集源自小肠的树突状细胞(DC)。我们用这种方法制备大鼠,并通过口服或肠内注射给予抗原。从这些动物在最初24小时内收集的胸导管淋巴中富集的DC能够在体外刺激致敏T细胞,并在足垫注射后启动腘窝淋巴结CD4 + T细胞,而来自同一胸导管淋巴的B细胞和T细胞在启动方面是无活性的。体外用抗原脉冲处理的500个或更少的DC能够在体内启动T细胞,而体外脉冲处理的B细胞或巨噬细胞数量多100倍则相当无活性。口服1 mg卵清蛋白足以负载DC用于T细胞的体内启动。在DC中不能直接检测到抗原,但在固有层的巨噬细胞中存在。通过向F1受体注射亲本DC并显示T细胞致敏受注射DC的主要组织相容性复合体限制,证明了DC向T细胞的直接抗原呈递。携带抗原的DC不会诱导可检测到的初次抗体反应,但在加强注射后可以检测到小的二次抗体反应。这些结果表明,DC在肠道中获取抗原的方式与体外或其他组织中发生的情况非常相似,这表明在粘膜表面处理抗原可能没有特殊差异。这些结果的一个含义是,旨在解释口服耐受性的假设必须考虑到接受口服抗原的动物中存在免疫刺激、携带抗原的DC。

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