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传导气道上皮中携带II类主要组织相容性复合体的树突状细胞的起源和稳态更新。

Origin and steady-state turnover of class II MHC-bearing dendritic cells in the epithelium of the conducting airways.

作者信息

Holt P G, Haining S, Nelson D J, Sedgwick J D

机构信息

Division of Cell Biology, Institute for Child Health Research, Perth, Australia.

出版信息

J Immunol. 1994 Jul 1;153(1):256-61.

PMID:8207240
Abstract

Recent studies have identified a contiguous network of class II MHC-bearing dendritic cells (DC) in the airway epithelium of several species, including humans. This network seems comparable to the epidermal Langerhans cell population, comprising up to 700 DC per mm2 of airway epithelium. Moreover, it accounts for virtually all local immunostaining for class II MHC, suggesting an important role in surveillance for inhaled Ag. This study examines the turnover of these airway DC using a radiation chimera model that uses congenic rats expressing different allotypic variants of CD45, detectable via mAbs. Steady-state bone marrow renewal of the airway DC population (which is continuously depleted by migration of mature cells to draining lymph nodes) was interrupted via x-irradiation or high-dose dexamethasone, after which the resident population declined by 85% over the ensuing 72 h. After transplantation with congenic bone marrow and an initial lag period for graft establishment, the airway DC population was rapidly restored to preirradiation levels. These findings indicate a half-life of < or = 2 days for airway epithelial DC. In contrast, epidermal Langerhans cell half-life was > or = 15 days. The only comparable (short) half-life previously reported for a peripheral tissue DC population, is that derived from the gut wall. This indicates that rapidly turning over DC populations are a unique feature of the major "mucosal" organ systems, which is consistent with these DC playing an important role in surveillance of mucosal tissues for incoming Ag.

摘要

最近的研究已经在包括人类在内的几种物种的气道上皮中确定了一个连续的、携带II类主要组织相容性复合体(MHC)的树突状细胞(DC)网络。这个网络似乎与表皮朗格汉斯细胞群体相似,每平方毫米气道上皮中包含多达700个DC。此外,它几乎占了所有II类MHC的局部免疫染色,表明其在监测吸入抗原方面发挥着重要作用。本研究使用辐射嵌合体模型来研究这些气道DC的更新情况,该模型使用了表达不同CD45同种异型变体的同基因大鼠,可通过单克隆抗体检测到。气道DC群体的稳态骨髓更新(成熟细胞迁移至引流淋巴结会使其持续减少)通过X射线照射或高剂量地塞米松被中断,在此之后,驻留群体在随后的72小时内下降了85%。在用同基因骨髓移植并经过初始的移植建立延迟期后,气道DC群体迅速恢复到照射前水平。这些发现表明气道上皮DC的半衰期≤2天。相比之下,表皮朗格汉斯细胞的半衰期≥15天。之前报道的唯一具有类似(短)半衰期的外周组织DC群体是来自肠壁的DC群体。这表明快速更新的DC群体是主要“黏膜”器官系统的一个独特特征,这与这些DC在监测黏膜组织中进入的抗原方面发挥重要作用是一致的。

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