调节人内皮细胞前列环素释放的组胺受体亚型的特性研究

Characterization of histamine receptor sub-types regulating prostacyclin release from human endothelial cells.

作者信息

Bull H A, Courtney P F, Rustin M H, Dowd P M

机构信息

Department of Dermatology, University College and Middlesex School of Medicine, London.

出版信息

Br J Pharmacol. 1992 Oct;107(2):276-81. doi: 10.1111/j.1476-5381.1992.tb12738.x.

DOI:10.1111/j.1476-5381.1992.tb12738.x

PMID:1330171

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1907870/

Abstract

The histamine receptor sub-types that are involved in the initiation and maintenance of prostacyclin (PGI2) release from human endothelial cells have been investigated. 2. Endothelial cells cultured from umbilical vein (HUVEC) were incubated with either histamine, the selective H1-receptor agonists, 2-methyl histamine (2-MeHA) or thiazolylethylamine (ThEA), the H1-agonist/H3-antagonist, beta-histidine (beta-His), the selective H2-agonist, dimaprit, the H2-agonist/H3-antagonist, impromidine, the selective H3-agonist, (R)alpha-methylhistamine ((R)alpha-MeHA) and the H3-antagonist, thioperamide. 3. The H1-agonists and the H3-agonist (R)alpha-MeHA induced a concentration (100 nM-1 mM) and time-dependent release of PGI2 as determined by radioimmunoassay for 6-keto-PGF1 alpha, but were less potent than histamine itself. The rank order of potency was the same following 30 min and 24 h incubation, i.e. histamine > ThEA > 2-MeHA >> beta-His > (R)alpha-MeHA. 4. Histamine and 2-MeHA (1 microM-1 mM), ThHEA (10 microM-1 mM) and (R)alpha-MeHA (1 mM), but not beta-His, induced a significantly greater increase in PGI2 release after 24 h incubation than after 30 min incubation (P < 0.05). 5. Neither the selective H2-agonist, dimaprit, nor the H2-agonist/H3-antagonist, impromidine alone induced release of PGI2. 6. The H1-antagonist, mepyramine (10 microM), abolished release of PGI2 induced by histamine, the H1-agonists and (R)alpha-MeHA but the H2-antagonist cimetidine (10 microM) and the H2/H3-antagonist, burimamide (10 microM) did not significantly modulate PGI2 release. 7. Although the H3-agonist (R)alphax-MeHA induced release of PGI2, it failed to modulate PGI2 release in the presence of histamine.8. Low concentrations of the H3-antagonist, thioperamide (100 nM) did not modulate histamine release of PGI2 at all but after 24 h incubation, thioperamide (10-4 M) partially reduced PGI2 release in the presence of histamine.9. These results indicate that PGI2 from HUVEC is initiated and maintained via histamine HI-receptor occupancy. There appears to be no involvement of either H2- or H3-receptors in this particular endothelial cell histaminergic response.

摘要

研究了参与人内皮细胞释放前列环素（PGI2）起始和维持过程的组胺受体亚型。2. 将从脐静脉培养的内皮细胞（HUVEC）与组胺、选择性H1受体激动剂2-甲基组胺（2-MeHA）或噻唑基乙胺（ThEA）、H1激动剂/H3拮抗剂β-组胺（β-His）、选择性H2激动剂地马普明、H2激动剂/H3拮抗剂英普咪定、选择性H3激动剂（R）α-甲基组胺（（R）α-MeHA）以及H3拮抗剂硫代丙酰胺一起孵育。3. 通过放射免疫分析法测定6-酮-PGF1α，发现H1激动剂和H3激动剂（R）α-MeHA在100 nM - 1 mM浓度范围内诱导PGI2呈浓度和时间依赖性释放，但效力低于组胺本身。孵育30分钟和24小时后效力顺序相同，即组胺＞ThEA＞2-MeHA＞＞β-His＞（R）α-MeHA。4. 组胺和2-MeHA（1μM - 1 mM）、ThHEA（10μM - 1 mM）以及（R）α-MeHA（1 mM），而非β-His，在孵育24小时后诱导的PGI2释放增加显著大于孵育30分钟后（P＜0.05）。5. 选择性H2激动剂地马普明和H2激动剂/H3拮抗剂英普咪定单用均未诱导PGI2释放。6. H1拮抗剂美吡拉敏（10μM）可消除组胺、H1激动剂和（R）α-MeHA诱导的PGI2释放，但H2拮抗剂西咪替丁（10μM）和H2/H3拮抗剂布立马胺（10μM）对PGI2释放无显著调节作用。7. 尽管H3激动剂（R）α-MeHA诱导了PGI2释放，但在存在组胺的情况下它未能调节PGI2释放。8. 低浓度的H3拮抗剂硫代丙酰胺（100 nM）对组胺诱导的PGI2释放完全无调节作用，但孵育24小时后，硫代丙酰胺（10 - 4M）在存在组胺的情况下部分降低了PGI2释放。9. 这些结果表明，HUVEC释放的PGI2是通过组胺H1受体占据起始并维持的。在这种特定的内皮细胞组胺能反应中，似乎不存在H2或H3受体的参与。