肺肥大细胞的独特群体是抗原介导的支气管收缩所必需的。
Unique populations of lung mast cells are required for antigen-mediated bronchoconstriction.
机构信息
Curriculum in Genetics and Molecular Biology Department of Medicine, Division of Pulmonary and Critical Care Medicine, University of North Carolina at Chapel Hill, Chapel Hill, NC 27599, USA.
出版信息
Clin Exp Allergy. 2011 Feb;41(2):260-9. doi: 10.1111/j.1365-2222.2010.03583.x. Epub 2010 Aug 16.
BACKGROUND
Studies in both human and mouse indicate that mediators released by mast cells can lead to bronchoconstriction, and thus these are important effector cells in lifethreatening anaphylaxis. Much of our understanding of the various functions of mast cells emanates from the study of mice lacking these cells, particularly mice carrying mutations in the tyrosine kinase gene Kit. Definitive evidence for the role of mast cells in the altered immune response requires the demonstration that this response can be normalized by reconstitution of the mice with cultured bone marrow-derived mast cells (BMMCs). While many mast cell niches can be restored with BMMCs, this has not been demonstrated for mast cells present in the airways of the lung, cells poised to mediate bronchoconstriction during allergic responses.
OBJECTIVE
To determine if mast cell-deficient Kit(Wsh/Wsh) reconstituted lines are an appropriate model for the study of the role of these cells in bronchoconstriction associated with allergic responses.
METHODS
Kit(Wsh/Wsh) mice were reconstituted with either whole bone marrow (WBM) or BMMCs and responses to IgE-mediated mast cell activation were determined; including systemic hypothermia, mediator release, and bronchoconstriction in anaesthetized, mechanically ventilated animals.
RESULTS
Engraftment of Kit(Wsh/Wsh) mice with WBM and BMMCs results in reconstitution of the central airways with mast cells. While the treatment of the two groups of animals resulted in systemic changes when challenged with IgE/Ag in a model of passive anaphylaxis, bronchoconstriction was observed only in kit(Wsh/Wsh) animals, which had received a bone marrow transplant.
CONCLUSIONS
While BMMCs can populate the lung, they cannot restore IgE/Ag-mediated bronchoconstriction to mast cell-deficient animals. This suggests that the mast cell population, which mediates this function, may be unique, and to fill this niche in the lung cells must undergo a specific developmental programme, one that is no longer available to cultured mast cells.
背景
人体和小鼠的研究表明,肥大细胞释放的介质可导致支气管收缩,因此这些细胞是危及生命的过敏反应中的重要效应细胞。我们对肥大细胞各种功能的理解主要来自于缺乏这些细胞的小鼠研究,尤其是携带酪氨酸激酶基因 Kit 突变的小鼠。要确定肥大细胞在改变的免疫反应中的作用,需要证明通过用培养的骨髓衍生的肥大细胞(BMMC)重建小鼠可以使这种反应正常化。虽然许多肥大细胞龛可以用 BMMC 来恢复,但尚未证明在肺气道中存在的肥大细胞,即在过敏反应期间介导支气管收缩的细胞中存在这种情况。
目的
确定肥大细胞缺陷型 Kit(Wsh/Wsh)重建系是否是研究这些细胞在与过敏反应相关的支气管收缩中的作用的合适模型。
方法
用全骨髓(WBM)或 BMMC 重建 Kit(Wsh/Wsh) 小鼠,并确定 IgE 介导的肥大细胞激活的反应;包括在麻醉、机械通气的动物中全身低温、介质释放和支气管收缩。
结果
用 WBM 和 BMMC 移植 Kit(Wsh/Wsh) 小鼠可使中央气道重建为肥大细胞。虽然两组动物在被动过敏反应模型中用 IgE/Ag 刺激时都会引起全身变化,但只有接受骨髓移植的 Kit(Wsh/Wsh) 动物才会观察到支气管收缩。
结论
虽然 BMMC 可以在肺部定植,但它们不能将 IgE/Ag 介导的支气管收缩恢复到肥大细胞缺陷型动物中。这表明介导这种功能的肥大细胞群体可能是独特的,并且要填补肺部的这个龛位,细胞必须经历特定的发育程序,而这种程序对于培养的肥大细胞来说已经不再可用。
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