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诱导黏膜免疫的细胞和分子机制。

Cellular and molecular mechanisms for induction of mucosal immunity.

作者信息

Brandtzaeg P, Farstad I N, Haraldsen G, Jahnsen F L

机构信息

Laboratory for Immunohistochemistry and Immunopathology (LIIPAT), University of Oslo, National Hospital, Norway.

出版信息

Dev Biol Stand. 1998;92:93-108.

PMID:9554262
Abstract

The epithelial glycoprotein called secretory component (SC) is quantitatively the most important receptor of the immune system because it is responsible for external transport of locally produced polymeric IgA (pIgA) to generate remarkably large amounts of secretory IgA. Antibodies of this type constitute the major mediators of specific humoral immunity. Transmembrane SC belongs to the Ig supergene family and functions as a common pIg receptor, also translocating pentameric IgM externally to form secretory IgM. The B cells responsible for mucosal production of Ig polymers are initially stimulated in organized mucosa-associated lympho-epithelial structures, particularly the Peyer's patches in the distal small intestine; from these inductive sites they migrate ("home") as memory cells to exocrine tissues all over the body. Mucous membranes are thus furnished with secretory antibodies in an integrated way, ensuring a variety of specificities at every secretory effector site. There is currently great interest in exploiting this integrated or "common" mucosal immune system for oral vaccination against pathogenic infectious agents and also to induce tolerance in T cell-mediated auto-immune diseases. However, much remains to be learned about mechanisms for antigen uptake and processing necessary to elicit stimulatory or suppressive mucosal immune responses in humans. Moreover, evidence is emerging for the existence of considerable regionalization with regard to functional links between inductive sites and effector sites of mucosal immunity.

摘要

被称为分泌成分(SC)的上皮糖蛋白在数量上是免疫系统最重要的受体,因为它负责将局部产生的聚合免疫球蛋白A(pIgA)向外转运,从而产生大量的分泌型免疫球蛋白A。这类抗体构成了特异性体液免疫的主要介质。跨膜SC属于免疫球蛋白超基因家族,作为一种常见的pIg受体发挥作用,还能将五聚体免疫球蛋白M转运至体外形成分泌型免疫球蛋白M。负责黏膜Ig聚合物产生的B细胞最初在有组织的黏膜相关淋巴上皮结构中受到刺激,特别是远端小肠的派尔集合淋巴结;它们作为记忆细胞从这些诱导部位迁移(“归巢”)到全身的外分泌组织。黏膜因此以一种整合的方式配备了分泌性抗体,确保每个分泌效应部位具有多种特异性。目前,人们对利用这种整合的或“共同的”黏膜免疫系统进行口服疫苗接种以对抗致病性感染因子以及在T细胞介导的自身免疫性疾病中诱导耐受性非常感兴趣。然而,关于在人类中引发刺激性或抑制性黏膜免疫反应所需的抗原摄取和加工机制,仍有许多需要了解的地方。此外,越来越多的证据表明,黏膜免疫的诱导部位和效应部位之间的功能联系存在相当大的区域化。

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