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内源性组胺在血管生成中的双重作用证据。

Evidence of a dual role of endogenous histamine in angiogenesis.

作者信息

Norrby K

机构信息

Department of Pathology, University of Göteborg, Sahlgrenska University Hospital, Sweden.

出版信息

Int J Exp Pathol. 1995 Apr;76(2):87-92.

Abstract

The specific activation of mast cells in situ causes vigorous local mast-cell mediated angiogenesis (MCMA). The mast cell is a major source of histamine and, as recently reported, specific histamine H1- and H2-membrane receptor antagonists are able individually to significantly suppress MCMA in rats, as assessed using the mesenteric window angiogenesis assay (MWAA). In addition to membrane receptors for histamine, a type of intracellular histamine receptors, designated Hic, has been described. It is now demonstrated that the potent Hic-receptor antagonist DPPE (N,N-diethyl-2-[4-(phenylmethyl)phenoxy]ethanamine HCl), administered parenterally, stimulates MCMA significantly in rats, as quantified by the MWAA. Although the target cell(s) are not known, there are several ways by which their Hic receptors could be activated: uptake of histamine released from mast cells, mobilization from preformed cytoplasmic and nuclear stores, and production of de novo histamine by histidine decarboxylase activity. The fact that the occupancy by histamine of H1- and H2-membrane receptors stimulates MCMA and the occupancy by histamine of Hic inhibits MCMA suggests that endogenous histamine is capable of regulating angiogenesis by a dual mode of action. This is apparently the first report ascribing a dual role of this type in angiogenesis to a single molecule.

摘要

肥大细胞在原位的特异性激活会引发强烈的局部肥大细胞介导的血管生成(MCMA)。肥大细胞是组胺的主要来源,并且正如最近报道的那样,使用肠系膜窗血管生成测定法(MWAA)评估发现,特异性组胺H1和H2膜受体拮抗剂能够分别显著抑制大鼠的MCMA。除了组胺膜受体外,还描述了一种细胞内组胺受体,称为Hic。现已证明,通过胃肠外给药的强效Hic受体拮抗剂DPPE(N,N - 二乙基 - 2 - [4 - (苯甲基)苯氧基]乙胺盐酸盐),通过MWAA定量分析,在大鼠中能显著刺激MCMA。虽然靶细胞尚不清楚,但有几种方式可激活其Hic受体:摄取肥大细胞释放的组胺、从预先形成的细胞质和核储存中动员以及通过组氨酸脱羧酶活性从头合成组胺。组胺占据H1和H2膜受体刺激MCMA,而组胺占据Hic抑制MCMA这一事实表明,内源性组胺能够通过双重作用模式调节血管生成。这显然是首次将这种类型的双重作用归因于单一分子在血管生成中的报道。

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