Visser Loes E, Penning-van Bees Fernie J A, Kasbergen A A Harrie, De Smet Peter A G M, Vulto Arnold G, Hofman Albert, Stricker Bruno H Ch
Pharmacoepidemiology Unit, Department of Internal Medicine, Erasmus University Medical Centre Rotterdam, Rotterdam, The Netherlands.
Thromb Haemost. 2002 Nov;88(5):705-10.
Several case reports associated combined use of coumarins and antibacterial drugs with overanticoagulation. Despite the fact that these drugs are frequently prescribed concurrently, there is little quantitative information on the risks of such complications.
To study which antibacterial drugs are associated with overanticoagulation during therapy with coumarins.
Population-based cohort study in a sample of the Rotterdam Study.
All patients who were treated with acenocoumarol or phenprocoumon in the study period from April 1, 1991 through December 31, 1998 and for whom INR data were available.
Patients were followed until an INR >/= 6.0, the end of their treatment, death or end of the study period. Proportional hazards regression analysis was used to estimate the risk of an INR >/= 6.0 in relation to concomitant use of an oral anticoagulant and antibacterial drugs after adjustment for several potentially confounding factors such as age, gender, hepatic dysfunction, malignancies, and heart failure.
Of the 1,124 patients in the cohort, 351 developed an INR >/= 6.0. The incidence rate was 6.9 per 10,000 treatment days. Sulfamethoxazole combined with trimethoprim most strongly increased the risk of overanticoagulation with an adjusted relative risk of 20.1 (95% CI: 10.7-37.9). Stratification showed that the induction period of overanticoagulation varied between different antibacterial drugs.
In this study among outpatients of an anticoagulation clinic using acenocoumarol or phenprocoumon, several antibacterial drugs strongly increased the risk of overanticoagulation. Awareness of these drug interactions and more frequent monitoring of INR values during the initial stages of antibacterial drug therapy are warranted to minimize the risk of bleeding complications.
数例病例报告将香豆素类药物与抗菌药物的联合使用与抗凝过度联系起来。尽管这些药物经常同时开具处方,但关于此类并发症风险的定量信息却很少。
研究在香豆素类药物治疗期间,哪些抗菌药物与抗凝过度有关。
基于鹿特丹研究样本的人群队列研究。
1991年4月1日至1998年12月31日研究期间接受醋硝香豆素或苯丙香豆素治疗且有国际标准化比值(INR)数据的所有患者。
对患者进行随访,直至INR≥6.0、治疗结束、死亡或研究期结束。在对年龄、性别、肝功能不全、恶性肿瘤和心力衰竭等几个潜在混杂因素进行调整后,使用比例风险回归分析来估计口服抗凝药与抗菌药物联合使用时INR≥6.0的风险。
队列中的1124名患者中,351名患者的INR≥6.0。发病率为每10000个治疗日6.9例。磺胺甲恶唑联合甲氧苄啶最显著增加抗凝过度风险,调整后的相对风险为20.1(95%置信区间:10.7 - 37.9)。分层分析表明,不同抗菌药物导致抗凝过度的诱导期有所不同。
在这项针对使用醋硝香豆素或苯丙香豆素的抗凝门诊患者的研究中,几种抗菌药物显著增加了抗凝过度的风险。认识到这些药物相互作用,并在抗菌药物治疗初期更频繁地监测INR值,对于将出血并发症风险降至最低是必要的。