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噻氯匹定对隐静脉搭桥通畅率的影响:一项双盲研究。

Effect of ticlopidine on saphenous vein bypass patency rates: a double-blind study.

作者信息

Chevigné M, David J L, Rigo P, Limet R

出版信息

Ann Thorac Surg. 1984 May;37(5):371-8. doi: 10.1016/s0003-4975(10)60757-6.

Abstract

The effects of ticlopidine, a new antiplatelet agent, on graft patency rate was investigated in a group of 150 consecutive patients undergoing aortocoronary bypass graft procedures. In a double-blind study, two groups of 75 patients each received ticlopidine (250 mg twice daily) or a placebo during a three-month period. Graft patency was evaluated by repeat angiography in 38 patients and by rest and stress myocardial scintigraphy in 93. Combined angiographic and scintigraphic analysis was performed in 36 patients. The biological effects of ticlopidine on platelet activity were assessed by bleeding time and appropriate ex vivo tests. Graft patency was evaluated in 131 patients (87%). Evaluation was performed at the end of the three-month therapy period in 77 patients (Groups T1 [ticlopidine] and P1 [placebo]) and five months later in 54 patients. The total graft attrition rate was 10.1% in Group T1 compared with 20.3% in Group P1 (p less than 0.1). Excluding patients with discordant biological data, the attrition rate was 7.1% for Group T1 compared with 21.8% for Group P1 (p less than 0.02). There was no difference between the subgroups evaluated five months after the end of therapy. Ticlopidine appears to be an effective means of protecting graft patency as long as the biological effects of the drug are present. This protective effect disappears when the drug is discontinued, which suggests that ticlopidine should be prescribed for a longer period, at least for the first year after operation.

摘要

在一组连续150例接受主动脉冠状动脉搭桥手术的患者中,研究了新型抗血小板药物噻氯匹定对移植血管通畅率的影响。在一项双盲研究中,两组各75例患者在三个月期间分别接受噻氯匹定(每日两次,每次250毫克)或安慰剂治疗。通过对38例患者进行重复血管造影以及对93例患者进行静息和负荷心肌闪烁显像来评估移植血管通畅情况。对36例患者进行了血管造影和闪烁显像的联合分析。通过出血时间和适当的体外试验评估噻氯匹定对血小板活性的生物学效应。对131例患者(87%)评估了移植血管通畅情况。在77例患者(T1组[噻氯匹定]和P1组[安慰剂])的三个月治疗期结束时进行了评估,54例患者在五个月后进行了评估。T1组的移植血管总损耗率为10.1%,而P1组为20.3%(p<0.1)。排除生物学数据不一致的患者后,T1组的损耗率为7.1%,而P1组为21.8%(p<0.02)。治疗结束五个月后评估的亚组之间没有差异。只要药物的生物学效应存在,噻氯匹定似乎是保护移植血管通畅的有效手段。当停药时这种保护作用消失,这表明噻氯匹定应开更长时间的处方,至少在术后第一年。

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