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炎症介质对豚鼠气道微血管通透性的区域和时间依赖性影响。

Regional and time-dependent effects of inflammatory mediators on airway microvascular permeability in the guinea pig.

作者信息

Evans T W, Rogers D F, Aursudkij B, Chung K F, Barnes P J

机构信息

Department of Thoracic Medicine, Cardiothoracic Institute, London.

出版信息

Clin Sci (Lond). 1989 May;76(5):479-85. doi: 10.1042/cs0760479.

Abstract
  1. Airway oedema resulting from increased microvascular permeability is a characteristic pathological finding of asthma. The regional effects of putative mediators involved in asthma on airway microvascular permeability have been studied. 2. The effects of histamine, leukotriene (LT) D4 and platelet-activating factor (PAF) on microvascular permeability in the nasal mucosa, larynx, trachea, main bronchi and intrapulmonary airways of the guinea pig were assessed by measuring the extravasation of intravenously administered Evans Blue dye. 3. PAF and LTD4 caused increased microvascular leakage throughout the respiratory tract, although their effects were maximal in different regions. Histamine had no significant effect on intrapulmonary airways. PAF was more potent than LTD4 and histamine at all airway levels. For example, in the trachea the doses required to cause leakage of 50% of maximal (ED50) were 10.4 nmol/kg, 138 nmol/kg and 11.2 mumol/kg, respectively, for PAF, LTD4 and histamine. 4. The effect of the three mediators was maximal 5 min after intravenous administration. Histamine, but neither LTD4 nor PAF, still caused significant leakage 30 min after administration. 5. The increased microvascular leakage induced by the mediators was inhibited by their respective specific receptor antagonists, suggesting that the effect was mediated via specific receptors. 6. Histamine, LTD4 and PAF have varying potencies in increasing microvascular permeability in the guinea-pig respiratory tract, exert their maximal effect in different regions and have varying durations of action.
摘要
  1. 微血管通透性增加导致的气道水肿是哮喘的典型病理表现。已对参与哮喘的假定介质对气道微血管通透性的局部作用进行了研究。2. 通过测量静脉注射伊文思蓝染料的外渗情况,评估组胺、白三烯(LT)D4和血小板活化因子(PAF)对豚鼠鼻黏膜、喉、气管、主支气管和肺内气道微血管通透性的影响。3. PAF和LTD4导致整个呼吸道微血管渗漏增加,尽管它们在不同区域的作用最大。组胺对肺内气道无显著影响。在所有气道水平,PAF比LTD4和组胺更有效。例如,在气管中,PAF、LTD4和组胺引起50%最大渗漏量(ED50)所需的剂量分别为10.4 nmol/kg、138 nmol/kg和11.2 μmol/kg。4. 静脉注射后5分钟,三种介质的作用最大。组胺在给药30分钟后仍导致显著渗漏,但LTD4和PAF则不然。5. 介质诱导的微血管渗漏增加被其各自的特异性受体拮抗剂抑制,表明该作用是通过特异性受体介导的。6. 组胺、LTD4和PAF在增加豚鼠呼吸道微血管通透性方面具有不同的效力,在不同区域发挥最大作用,且作用持续时间不同。

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