-
Title
- Safety and efficacy of ticlopidine for only 2 weeks after successful intracoronary
stent placement.
- Author
- Berger PB; Bell MR; Hasdai D; Grill DE; Melby S; Holmes DR Jr
- Address
- Division of Cardiovascular Diseases, Department of Internal Medicine and the Section
of Biostatistics, Mayo Clinic, Rochester, MN, USA. berger.peter@mayo.edu
- Source
- Circulation, 99(2):248-53 1999 Jan 19
- Abstract
- BACKGROUND: In patients receiving intracoronary stents, stent thrombosis is reduced
when ticlopidine therapy is combined with aspirin after the procedure. However, ticlopidine
causes neutropenia in 1% of patients when administered for >2 weeks, and little is
known about the duration that ticlopidine needs be administered to prevent stent
thrombosis. METHODS AND RESULTS: We analyzed 827 patients undergoing successful stent
placement in 1061 coronary segments at Mayo Clinic who were treated between May 1, 1996,
and October 31, 1997. Chronic warfarin therapy, cardiogenic shock, and enrollment in
research protocols requiring 4 weeks of ticlopidine were exclusion criteria; ticlopidine
was discontinued after 14 days in all remaining patients. The mean age of the study
population was 64+/-11 years; 49% had suffered a prior infarction, 20% had undergone
coronary artery bypass surgery, and 65% had multivessel disease. The indication for stent
placement was dissection or abrupt closure in 31% of patients and suboptimal results from
balloon angioplasty in 18%. Placement was elective in 51% of patients, and 10.3% of
patients were treated within 12 hours of an acute myocardial infarction. Mean nominal
stent size was 3.3+/-0.5 mm. High-pressure inflations (>/=12 atm) were performed in all
patients (mean, 17+/-4 atm). Intravascular ultrasound was used to facilitate stent
placement in 8.8% of patients. Abciximab was administered to 38% of patients; 11% of
patients who were at increased risk of stent thrombosis were treated with enoxaparin for
10 to 14 days. Adverse cardiovascular events in the 14 days after stent placement occurred
in 11 patients (1.3%). Two patients died of nonischemic causes (sepsis and renal failure)
in the 15th through 30th days after ticlopidine was stopped. However, there were no
cardiovascular deaths, myocardial infarctions, coronary artery bypass operations, or
repeat angioplasty procedures between the 15th and 30th days; stent thrombosis did not
occur in any patient after ticlopidine had been stopped. No patient developed
neutropenia, although 1.8% of the first 489 patients who were closely monitored for side
effects from ticlopidine developed side effects requiring its discontinuation, and
milder side effects occurred in 4.7%. CONCLUSIONS: In patients receiving intracoronary
stents, the discontinuation of ticlopidine therapy 14 days after stent placement is
associated with a very low frequency of stent thrombosis and other adverse events.