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拉氧头孢、头孢噻肟和头孢哌酮对正常志愿者血小板功能及凝血的影响。

The effects of latamoxef, cefotaxime, and cefoperazone on platelet function and coagulation in normal volunteers.

作者信息

Weitekamp M R, Caputo G M, Al-Mondhiry H A, Aber R C

出版信息

J Antimicrob Chemother. 1985 Jul;16(1):95-101. doi: 10.1093/jac/16.1.95.

Abstract

A bleeding diathesis characterized by in-vitro platelet dysfunction and prolongation of the template bleeding time (TBT) has been reported in patients receiving latamoxef ('moxalactam'), but not cefotaxime or cefoperazone. Hypoprothrombinaemia has been associated with the use of both latamoxef and cefoperazone in seriously ill and malnourished patients. We administered either latamoxef, cefotaxime or cefoperazone intravenously, at dosages within the range recommended by each manufacturer, to 14 normal volunteers. Latamoxef caused a dose and time dependent defect in platelet function characterized in vitro by abnormalities in aggregation to adenosine diphosphate and in vivo by prolongation of the template bleeding time. In two out of two subjects, a single 4 g dose of latamoxef caused neither prolongation of template bleeding times nor aggregation abnormalities. Two out of two subjects receiving latamoxef 6 g/day for six days had progressive prolongation of bleeding times to 12 and 15 min. Two additional subjects receiving latamoxef 12 g/day for four days had prolongation of template bleeding times to greater than 20 min. Of four subjects receiving cefotaxime 12 g/day for seven days, none had prolongation of template bleeding times or abnormalities in platelet aggregations. Of four subjects receiving cefoperazone 6 g/day, none had significant prolongation of template bleeding times and one had abnormalities in aggregation attributed to inadvertent salicylate ingestion. Prolongation of the prothrombin time or activated partial thromboplastin time did not occur in any of the 14 volunteers. Latamoxef is more likely to interfere with platelet function than either cefotaxime or cefoperazone.

摘要

据报道,接受拉氧头孢(“羟羧氧酰胺菌素”)治疗的患者会出现一种以体外血小板功能障碍和模板出血时间(TBT)延长为特征的出血素质,但接受头孢噻肟或头孢哌酮治疗的患者未出现这种情况。在重症和营养不良患者中,低凝血酶原血症与拉氧头孢和头孢哌酮的使用有关。我们将拉氧头孢、头孢噻肟或头孢哌酮按照各制造商推荐的剂量范围静脉注射给14名正常志愿者。拉氧头孢会导致剂量和时间依赖性的血小板功能缺陷,其体外特征为对二磷酸腺苷的聚集异常,体内特征为模板出血时间延长。在两名受试者中,单次4g剂量的拉氧头孢既未导致模板出血时间延长,也未出现聚集异常。两名受试者接受6g/天的拉氧头孢治疗6天,出血时间逐渐延长至12分钟和15分钟。另外两名受试者接受12g/天的拉氧头孢治疗4天,模板出血时间延长至20分钟以上。四名受试者接受12g/天的头孢噻肟治疗7天,无人出现模板出血时间延长或血小板聚集异常。四名受试者接受6g/天的头孢哌酮治疗,无人出现模板出血时间显著延长,一名受试者因意外摄入水杨酸盐出现聚集异常。14名志愿者中无一例出现凝血酶原时间或活化部分凝血活酶时间延长。与头孢噻肟或头孢哌酮相比,拉氧头孢更有可能干扰血小板功能。

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