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组胺的选择性嗜酸性粒细胞趋化活性。

The selective eosinophil chemotactic activity of histamine.

作者信息

Clark R A, Gallin J I, Kaplan A P

出版信息

J Exp Med. 1975 Dec 1;142(6):1462-76. doi: 10.1084/jem.142.6.1462.

Abstract

Histamine diphosphate was shown to selectively attract human eosinophils from mixed granulocyte populations when over 20% eosinophils were used in a modified Boyden chamber chemotactic assay system. This effect of histamine is abolished by incubation with diamine oxidase (histaminase) and was generated by decarboxylation of L-histidine. A linear dose dependent increase in eosinophil migration was observed between 3 X 10(-7) M and 1.25 X 10(-6) M, while higher concentrations of histamine inhibited the migration of eosinophils. The attractant activity of histamine was not inhibited by H-1 or H-2 receptor antagonists, however, the inhibition of migration observed at higher histamine concentrations was reversed by metiamine, an H-2 receptor antagonist. The effects of histamine upon eosinophil migration were demonstrable using three different assays: (a) counting cells that had traversed 5-mum pore, 12-mum thick polycarbonate filters, (b) counting cells that had migrated various distances into a 3-mum pore, 145-mum cellulose nitrate filters, or (c) measuring the number of cells that had traversed an upper polycarbonate filter and migrated into a lower cellulose nitrate filter using 15Cr-labeled cells. The ability of histamine to enhance eosinophil migration was shown to be dependent upon the presence of a concentration gradient; histamine did not cause a dose-dependent increase in random motility. Furthermore, preincubation of the eosinophils with histamine deactivate the cells to further stimulation by histamine or by C5a. It is concluded that in low doses histamine is a chemoattractant for human eosinophils, while in higher doses histamine inhibits eosinophil migration. These observations may relate to the influx and localization of eosinophils in immediate hypersensitivity reactions.

摘要

在改良的博伊登室趋化分析系统中,当使用超过20%的嗜酸性粒细胞时,二磷酸组胺可从混合粒细胞群体中选择性吸引人类嗜酸性粒细胞。组胺的这种作用可通过与二胺氧化酶(组胺酶)孵育而消除,且由L-组氨酸脱羧产生。在3×10⁻⁷ M至1.25×10⁻⁶ M之间观察到嗜酸性粒细胞迁移呈线性剂量依赖性增加,而更高浓度的组胺则抑制嗜酸性粒细胞的迁移。组胺的趋化活性不受H-1或H-2受体拮抗剂的抑制,然而,在较高组胺浓度下观察到的迁移抑制可被H-2受体拮抗剂甲硫咪胺逆转。使用三种不同的分析方法可证明组胺对嗜酸性粒细胞迁移的影响:(a) 计数穿过5μm孔径、12μm厚聚碳酸酯滤膜的细胞;(b) 计数迁移到3μm孔径、145μm硝酸纤维素滤膜不同距离的细胞;或(c) 使用¹⁵Cr标记的细胞测量穿过上层聚碳酸酯滤膜并迁移到下层硝酸纤维素滤膜的细胞数量。组胺增强嗜酸性粒细胞迁移的能力被证明取决于浓度梯度的存在;组胺不会导致随机运动的剂量依赖性增加。此外,嗜酸性粒细胞与组胺预孵育会使细胞对组胺或C5a的进一步刺激失活。得出的结论是,低剂量时组胺是人类嗜酸性粒细胞的趋化剂,而高剂量时组胺抑制嗜酸性粒细胞迁移。这些观察结果可能与速发型超敏反应中嗜酸性粒细胞的流入和定位有关。

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