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左旋特布他林可阻断血小板活化因子的炎症作用。

The inflammatory actions of platelet activating factor are blocked by levorotatory terbutaline.

作者信息

Dobbins D E, Buehn M J, Dabney J M

机构信息

Department of Physiology Uniformed Services University of the Health Sciences Bethesda, Maryland 20814-4799.

出版信息

Microcirc Endothelium Lymphatics. 1990 Dec;6(6):437-55.

PMID:1965987
Abstract

Platelet activating factor (PAF), a potent vasoactive lipid, may play an important role in the inflammatory process. In this study, we infused PAF intra-arterially to characterize its edematogenic potency in the canine forelimb. We have also assessed the ability of the beta 2-receptor agonist l-terbutaline to block PAF-mediated edema formation. The infusion of PAF at .25 micrograms/min, .5 micrograms/min and 1 micrograms/min increased forelimb arterial pressures and, at the two higher dosages, significantly decreased systemic arterial pressure. PAF infusions increased transvascular fluid and macromolecular flux as indicated by significant increases in skin lymph flow, protein concentration and protein transport. The intra-arterial infusion of l-terbutaline at 1 micrograms/min significantly decreased forelimb arterial pressures but did not affect small vein pressure, systemic pressure or forelimb lymph parameters. The subsequent infusion of PAF at .5 micrograms/min, during the continued infusion of l-terbutaline, failed to significantly affect forelimb lymph parameters. These data indicate that PAF is significantly more potent as an edematogenic agent in the forelimb than histamine or bradykinin. Furthermore, the blockade of PAF-mediated edema formation by l-terbutaline suggests that beta 2-receptor agonists may be capable of antagonizing the inflammatory actions of a wide variety of putative inflammatory mediators.

摘要

血小板活化因子(PAF)是一种强效血管活性脂质,可能在炎症过程中发挥重要作用。在本研究中,我们通过动脉内输注PAF来表征其在犬前肢的致水肿能力。我们还评估了β2受体激动剂l - 特布他林阻断PAF介导的水肿形成的能力。以0.25微克/分钟、0.5微克/分钟和1微克/分钟的速度输注PAF会增加前肢动脉压,并且在两个较高剂量时会显著降低体动脉压。PAF输注增加了跨血管液体和大分子通量,表现为皮肤淋巴流量、蛋白质浓度和蛋白质转运显著增加。以1微克/分钟的速度动脉内输注l - 特布他林可显著降低前肢动脉压,但不影响小静脉压、体循环压力或前肢淋巴参数。在持续输注l - 特布他林期间,随后以0.5微克/分钟的速度输注PAF未能显著影响前肢淋巴参数。这些数据表明,PAF作为前肢致水肿剂比组胺或缓激肽的效力显著更强。此外,l - 特布他林对PAF介导的水肿形成的阻断表明,β2受体激动剂可能能够拮抗多种假定的炎症介质的炎症作用。

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