用巨噬细胞-1(mac-1)抑制剂进行预处理可改变猪缺血再灌注期间局部和全身的血小板功能。
Pretreatment with an inhibitor of mac-1 alters regional and systemic platelet function during ischemia-reperfusion in swine.
作者信息
Gurbel P A, Serebruany V L, Komiathy S F, Collins M E, Bittar G D, Schlossberg M L, Mergner W
机构信息
Union Memorial Hospital, Baltimore, Md 21218, USA.
出版信息
Pharmacology. 1996 Aug;53(2):79-86. doi: 10.1159/000139418.
Myocardial ischemia-reperfusion alters regional and systemic platelet function. The aim of our study was to elucidate the role of the Mac-1 receptor in changes of platelet function by using the leumedin, NPC-15669, an inhibitor of Mac-1 upregulation. In an open-chest swine model (n = 15), the treatment group (n = 6) received NPC-15669 (10 mg/kg loading dose over 12 min at the rate of 5 ml/min at the onset of left-anterior descending coronary artery occlusion, followed by constant infusion at 6 mg kg-1 h-1 during 90 min of reperfusion). Regional platelet aggregation (response to 5 microM ADP) increased after 15 min occlusion (126% of baseline) and at 90 min of reperfusion (156% of baseline). This increase in platelet aggregability was inhibited by NPC-15669 (83% of baseline after 15 min occlusion and 98% of baseline at 90 min reperfusion, both p < 0.001 compared to control). Systemic platelet function was not affected by NPC-15669 after 15 min occlusion (102% of baseline vs. 96% of baseline for control, p = NS). At 90 min of reperfusion platelet function was increased in controls (131% of baseline) and not affected by NPC-15669 (126% of baseline, p = NS). Myocardial neutrophil accumulation did not differ between the control and treatment groups. Inhibition of Mac-1 upregulation by NPC-15669 attenuates the increased regional platelet aggregability resulting from myocardial ischemia-reperfusion, with a less marked effect on the systemic response. The data suggest that Mac-1 may modulate regional platelet responses induced by ischemia-reperfusion. The increased aggregability of platelets during ischemia and reperfusion and its attenuation by inhibition of Mac-1 may be relevant for future strategies to reduce coronary arterial occlusion by platelet thrombi.
心肌缺血再灌注会改变局部和全身的血小板功能。我们研究的目的是通过使用leumedin(NPC - 15669,一种抑制Mac - 1上调的抑制剂)来阐明Mac - 1受体在血小板功能变化中的作用。在一个开胸猪模型(n = 15)中,治疗组(n = 6)接受NPC - 15669(在左前降支冠状动脉闭塞开始时,以5毫升/分钟的速度在12分钟内给予10毫克/千克的负荷剂量,随后在90分钟的再灌注期间以6毫克·千克⁻¹·小时⁻¹的速度持续输注)。局部血小板聚集(对5微摩尔ADP的反应)在闭塞15分钟后(为基线的126%)和再灌注90分钟时(为基线的156%)增加。NPC - 15669抑制了血小板聚集性的这种增加(闭塞15分钟后为基线的83%,再灌注90分钟时为基线的98%,与对照组相比,两者p < 0.001)。闭塞15分钟后,NPC - 15669未影响全身血小板功能(与对照组相比,为基线的102%对96%,p = 无显著性差异)。在再灌注90分钟时,对照组的血小板功能增加(为基线的131%),而NPC - 15669未对其产生影响(为基线的126%,p = 无显著性差异)。对照组和治疗组之间心肌中性粒细胞的积聚没有差异。NPC - 15669对Mac - 1上调的抑制减弱了心肌缺血再灌注导致的局部血小板聚集性增加,对全身反应的影响较小。数据表明,Mac - 1可能调节缺血再灌注诱导的局部血小板反应。缺血和再灌注期间血小板聚集性的增加以及通过抑制Mac - 1对其的减弱可能与未来减少血小板血栓导致冠状动脉闭塞的策略相关。
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