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血小板活化因子在IgE致敏大鼠中抗原诱导的晚期气道微血管渗漏中的作用

Role of PAF in the late airway microvascular leakage induced by antigen in IgE-sensitized rat.

作者信息

Kyriacopoulos F, Boichot E, Lagente V, Mencia-Huerta J M, Braquet P

机构信息

Institut Henri Beaufour, Les Ulis, France.

出版信息

Fundam Clin Pharmacol. 1995;9(4):350-6. doi: 10.1111/j.1472-8206.1995.tb00509.x.

Abstract

The effect of the antagonist of platelet-activating factor (PAF), BN 50730, on PAF-and antigen- induced increase in microvascular leakage, using Evans blue dye as an index of permeability, was investigated in rat pulmonary tissues. PAF (1 microgram/kg, iv) induced a marked increase in Evans blue dye content in trachea, main bronchi and small bronchi, that was significantly reduced upon pretreatment of the rats with BN 50730 (25 mg/kg, orally) and by the serotonin antagonist, methysergide (1 mg/kg, iv), only in the small bronchi. Serotonin also induced an increase in microvascular leakage in the three tissues that was significantly inhibited when the animals were treated with methysergide but not by BN 50730. In contrast, histamine and lyso-PAF did not induce significant increase in Evans blue dye content. Intravenous injection of antigen to IgE-sensitized rats induced a biphasic increase in vascular permeability. An early increase in vascular permeability in trachea, main bronchi and small bronchi was observed 10 minutes after the injection of the antigen, and this phenomenon was significantly reduced upon treatment of the rats with methysergide, whereas, BN 50730 was ineffective. A late increase in vascular permeability was noted in the three tissues, with a maximum at 120 minutes and representing 30-40% of the magnitude of the first phase. Administration of BN 50730 (25 mg/kg) to the animals, evoked a significant inhibition of this increase in microvascular leakage, whereas, methysergide only significantly reduced the one induced by antigen in the trachea.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

以伊文思蓝染料作为通透性指标,研究了血小板活化因子(PAF)拮抗剂BN 50730对PAF和抗原诱导的大鼠肺组织微血管渗漏增加的影响。PAF(1微克/千克,静脉注射)可使气管、主支气管和小支气管中的伊文思蓝染料含量显著增加,而在大鼠预先口服BN 50730(25毫克/千克)和静脉注射5-羟色胺拮抗剂美西麦角(1毫克/千克)后,仅小支气管中的这种增加显著减少。5-羟色胺也可诱导这三种组织中的微血管渗漏增加,当动物用美西麦角治疗时,这种增加被显著抑制,但BN 50730无此作用。相比之下,组胺和溶血PAF未诱导伊文思蓝染料含量显著增加。向IgE致敏大鼠静脉注射抗原可诱导血管通透性出现双相增加。注射抗原10分钟后,观察到气管、主支气管和小支气管的血管通透性早期增加,用美西麦角治疗大鼠后,这种现象显著减少,而BN 50730无效。在这三种组织中均观察到血管通透性后期增加,在120分钟时达到最大值,为第一阶段幅度的30%-40%。给动物施用BN 50730(25毫克/千克)可显著抑制这种微血管渗漏增加,而美西麦角仅显著降低抗原在气管中诱导的增加。(摘要截断于250字)

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