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Mast-cell histamine is angiogenic through receptors for histamine1 and histamine2.

机译:肥大细胞组胺通过组胺1和组胺2的受体具有血管生成作用。

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摘要

The activation of mast-cells in situ induces angiogenesis in normally vascularized, adult mammalian tissue. Since the secreting mast-cell characteristically releases histamine, we studied the possible role of histamine in the outcome of mast-cell mediated angiogenesis using the rat mesenteric window assay. One H1-receptor antagonist, brompheniramine maleate (BPA), and one H2-receptor antagonist, metiamide, were separately administered systemically (s.c.) at non-toxic doses during the period of angiogenesis induction. Angiogenesis was effected by i.p. injections of the mast-cell secretagogue compound 48/80 for 5 consecutive days. The animals were killed 14 days after the start of the i.p. and s.c. treatment, close to the middle of the expanding angiogenic phase of the angiogenic reaction studied. Angiogenesis was quantified in terms of (a) the number of vessel profiles per unit tissue length (No/UL), which reflects mainly the degree of branching and/or tortuosity, (b) the relative vascularized area (VA), which is a measure of spatial extension, and (c) the vascular density (VD), a measure of vessel density per unit area of vascularized tissue. Whereas BPA significantly suppressed No/UL, metiamide significantly reduced No/UL and VD in statistical terms suggesting that endogenous mast-cell histamine is angiogenic through both H1- and H2-receptors. This appears to be the first paper to report that the occupancy of H2-receptors is angiogenic.
机译:肥大细胞的原位活化在正常血管化的成年哺乳动物组织中诱导血管生成。由于分泌的肥大细胞特征性地释放组胺,因此我们使用大鼠肠系膜窗试验研究了组胺在肥大细胞介导的血管生成结果中的可能作用。在血管生成诱导期间,以无毒剂量分别全身(皮下)施用一种H1受体拮抗剂马来酸溴苯那敏(BPA)和一种H2受体拮抗剂甲米酰胺。血管生成受腹膜内注射影响。连续5天注射肥大细胞促分泌素化合物48/80。腹腔注射开始后14天将动物处死。和s.c.在治疗中,已接近对血管生成反应的扩展血管生成阶段的中间进行研究。血管生成的量化依据是:(a)每单位组织长度的血管分布图数量(No / UL),这主要反映分支和/或曲折程度,(b)相对血管化面积(VA),即(a)血管密度(VD),衡量血管扩张组织每单位面积的血管密度。 BPA显着抑制No / UL,而甲酰胺在统计学上显着降低No / UL和VD,表明内源性肥大细胞组胺通过H1和H2受体均具有血管生成作用。这似乎是第一篇报道H2受体具有血管生成作用的论文。

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