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小鼠免疫应答诱导过程中肥大细胞的活化及向淋巴结的迁移。

Mast cell activation and migration to lymph nodes during induction of an immune response in mice.

作者信息

Wang H W, Tedla N, Lloyd A R, Wakefield D, McNeil P H

机构信息

Inflammation Research Unit, School of Pathology, University of New South Wales, Sydney, 2052 Australia.

出版信息

J Clin Invest. 1998 Oct 15;102(8):1617-26. doi: 10.1172/JCI3704.

Abstract

The mast cell response in skin and lymph nodes was examined during the sensitization phase of dinitrofluorobenzene (DNFB)-induced contact hypersensitivity in mice. Degranulation of 62% of mast cells in DNFB-exposed skin was evident within 30 min of a dual application of DNFB, reaching a peak of 77% at 24 h, and persisting in 42% after 5 d. Abundant expression of macrophage inflammatory protein (MIP)-1alpha and MIP-1beta mRNAs and proteins was observed in keratinocytes, and mast cell degranulation was significantly inhibited after administration of neutralizing antibodies to MIP-1alpha, but not MIP-1beta. During DNFB sensitization, the mast cell density in the skin decreased by half, concurrent with a fivefold expansion of mast cell numbers in draining lymph nodes. Fluorescent-labeled mast cells injected into the skin appeared in draining lymph nodes after application of DNFB, followed by subsequent migration to the spleen. In lymph nodes, mast cells were an abundant and predominant source of MIP-1beta, neutralization of which partially inhibited T lymphocyte recruitment. These results indicate that mast cells contribute to the induction of this primary immune response by activation at and migration from the site of antigen encounter to draining lymph nodes, wherein they mediate T lymphocyte recruitment by production of MIP-1beta.

摘要

在二硝基氟苯(DNFB)诱导的小鼠接触性超敏反应致敏阶段,检测了皮肤和淋巴结中的肥大细胞反应。在重复涂抹DNFB后30分钟内,暴露于DNFB的皮肤中62%的肥大细胞明显脱颗粒,24小时时达到峰值77%,5天后仍有42%的肥大细胞脱颗粒。在角质形成细胞中观察到巨噬细胞炎性蛋白(MIP)-1α和MIP-1β mRNA及蛋白的大量表达,给予抗MIP-1α中和抗体后,肥大细胞脱颗粒受到显著抑制,但抗MIP-1β中和抗体则无此作用。在DNFB致敏过程中,皮肤中的肥大细胞密度降低一半,同时引流淋巴结中的肥大细胞数量增加了五倍。将荧光标记的肥大细胞注入皮肤后,涂抹DNFB后其出现在引流淋巴结中,随后迁移至脾脏。在淋巴结中,肥大细胞是MIP-1β的丰富且主要来源,中和MIP-1β可部分抑制T淋巴细胞募集。这些结果表明,肥大细胞通过在抗原接触部位被激活并从该部位迁移至引流淋巴结,从而促进这种初次免疫反应的诱导,在淋巴结中它们通过产生MIP-1β介导T淋巴细胞募集。

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