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特定血小板活化因子拮抗剂对主动致敏豚鼠肺脏对血小板活化因子自身高反应性的有限干扰。

Limited interference of specific Paf antagonists with hyper-responsiveness to Paf itself of lungs from actively sensitized guinea-pigs.

作者信息

Pretolani M, Lefort J, Vargaftig B B

机构信息

Unité de Pharmacologie Cellulaire/Unité Associée Institut Pasteur-INSERM, Paris, France.

出版信息

Br J Pharmacol. 1989 Jun;97(2):433-42. doi: 10.1111/j.1476-5381.1989.tb11970.x.

DOI:10.1111/j.1476-5381.1989.tb11970.x
PMID:2474345
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1854509/
Abstract
  1. The interference of various platelet-activating factor (Paf) antagonists with Paf- and antigen-induced effects in isolated lungs from actively sensitized guinea-pigs was investigated. 2. WEB 2086 and BN 52021, two antagonists structurally unrelated to Paf, at concentrations 10-100 fold above those exerting a potent and selective inhibition of the effects of Paf in lungs from non-immunized guinea-pigs, failed to inhibit bronchoconstriction and mediator release evoked by the phospholipid when administered into lungs from actively sensitized animals. 3. In contrast to WEB 2086 and BN 52021, antagonists such as Ro 19-3704 and Ro 19-1400, structurally related to the Paf molecule, at concentrations which abrogate the effects of Paf in lungs from non-immunized guinea-pigs, inhibited bronchoconstriction and release of histamine and leukotriene-like material evoked by the intra-arterial administration of Paf into lungs from actively sensitized animals. 4. Ro 19-3704 and Ro 19-1400 also inhibited markedly the release of leukotriene C4 (LTC4)-like material and, to a smaller extent, the histamine secretion induced by 10 micrograms arachidonic acid. 5. CV 6209, another Paf antagonist structurally related to the phospholipid, failed to antagonize its bronchopulmonary and secretory effects in sensitized lungs. 6. All the antagonists used, irrespective of their ability to interfere or not with bronchoconstriction and mediator release triggered by Paf, suppressed oedema formation as measured by the increase in lung wet weight induced by either Paf or ovalbumin. 7. Our results indicate that: (i) the increase in vascular permeability and the subsequent oedema formation on one hand and the bronchopulmonary effects of Paf on the other hand are mediated by different mechanisms; and (ii) active sensitization provokes a marked modification of the lung reactivity to Paf.
摘要
  1. 研究了多种血小板活化因子(Paf)拮抗剂对主动致敏豚鼠离体肺中Paf和抗原诱导效应的干扰作用。2. WEB 2086和BN 52021这两种与Paf结构无关的拮抗剂,其浓度比在非免疫豚鼠肺中对Paf效应产生有效且选择性抑制作用时的浓度高10至100倍,当将其注入主动致敏动物的肺中时,未能抑制磷脂诱发的支气管收缩和介质释放。3. 与WEB 2086和BN 52021不同,诸如Ro 19 - 3704和Ro 19 - 1400等与Paf分子结构相关的拮抗剂,在消除非免疫豚鼠肺中Paf效应的浓度下,可抑制主动致敏动物肺中经动脉注射Paf所诱发的支气管收缩以及组胺和白三烯样物质的释放。4. Ro 19 - 3704和Ro 19 - 1400还显著抑制白三烯C4(LTC4)样物质的释放,并在较小程度上抑制由10微克花生四烯酸诱导的组胺分泌。5. CV 6209是另一种与磷脂结构相关的Paf拮抗剂,未能拮抗其在致敏肺中的支气管肺和分泌效应。6. 所有使用的拮抗剂,无论其是否能够干扰Paf触发的支气管收缩和介质释放,均能抑制通过Paf或卵清蛋白诱导的肺湿重增加所测量的水肿形成。7. 我们的结果表明:(i)一方面血管通透性增加及随后的水肿形成与另一方面Paf的支气管肺效应是由不同机制介导的;(ii)主动致敏引起肺对Paf反应性的显著改变。

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Limited interference of specific Paf antagonists with hyper-responsiveness to Paf itself of lungs from actively sensitized guinea-pigs.特定血小板活化因子拮抗剂对主动致敏豚鼠肺脏对血小板活化因子自身高反应性的有限干扰。
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引用本文的文献

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Paf. A mediator in search of a disease.
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PAF. A review of its effects, antagonists and possible future clinical implications (Part II).血小板活化因子。其作用、拮抗剂及未来可能的临床意义综述(第二部分)
Drugs. 1991 Aug;42(2):174-204. doi: 10.2165/00003495-199142020-00002.
3
Platelet activating factor and systemic anaphylaxis in Nippostrongylus brasiliensis-sensitized rats: differential effects of PAF antagonists.巴西日圆线虫致敏大鼠中的血小板活化因子与全身性过敏反应:血小板活化因子拮抗剂的不同作用
Br J Pharmacol. 1992 Jun;106(2):263-6. doi: 10.1111/j.1476-5381.1992.tb14326.x.
4
Interference of BN 52021, an antagonist of PAF, with different forms of active anaphylaxis in the guinea-pig: importance of the booster injection.血小板活化因子拮抗剂BN 52021对豚鼠不同形式主动过敏反应的干扰:加强注射的重要性
Br J Pharmacol. 1991 Mar;102(3):687-95. doi: 10.1111/j.1476-5381.1991.tb12234.x.

本文引用的文献

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A method for the fluorometric assay of histamine in tissues.一种用于组织中组胺荧光测定的方法。
J Pharmacol Exp Ther. 1959 Nov;127:182-6.
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Release of leukotriene C4 from human polymorphonuclear leucocytes as determined by radioimmunoassay.通过放射免疫测定法测定人多形核白细胞中白三烯C4的释放。
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The platelet-independent release of thromboxane A2 by Paf-acether from guinea-pig lungs involves mechanisms distinct from those for leukotriene.血小板激活因子从豚鼠肺中释放血栓素A2不依赖血小板,其机制与白三烯不同。
Br J Pharmacol. 1984 Jul;82(3):565-75. doi: 10.1111/j.1476-5381.1984.tb10795.x.
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CV-3988 - a specific antagonist of platelet activating factor (PAF).CV - 3988——一种血小板活化因子(PAF)的特异性拮抗剂。
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8
Interference by the novel PAF-acether antagonist WEB 2086 with the bronchopulmonary responses to PAF-acether and to active and passive anaphylactic shock in guinea-pigs.新型血小板活化因子拮抗剂WEB 2086对豚鼠支气管肺脏对血小板活化因子、主动及被动过敏反应性休克反应的干扰作用。
Eur J Pharmacol. 1987 Aug 21;140(3):311-21. doi: 10.1016/0014-2999(87)90288-3.
9
Pharmacological actions of WEB 2086, a new specific antagonist of platelet activating factor.血小板活化因子新型特异性拮抗剂WEB 2086的药理作用
J Pharmacol Exp Ther. 1987 Jun;241(3):974-81.
10
Airway epithelium modulates the reactivity of guinea-pig respiratory smooth muscle.气道上皮调节豚鼠呼吸道平滑肌的反应性。
Eur J Pharmacol. 1986 Sep 23;129(1-2):11-8. doi: 10.1016/0014-2999(86)90330-4.