MUNICH—The investigational antiplatelet drug prasugrel was particularly effective for cutting ischemic events in patients with diabetes and relatively less effective in patients without diabetes in a prespecified analysis of the more than 13,000 patients in the drug's pivotal trial.
Initial results reported in November 2007 from the Trial to Assess Improvements in Therapeutic Outcomes by Optimizing Platelet Inhibition with Prasugrel-Thrombolysis in Myocardial Infarction 38 (TRITON-TIMI-38) showed that in moderate- to high-risk patients with acute coronary syndrome who were scheduled to undergo percutaneous coronary intervention treatment with prasugrel led to a 19% relative risk reduction in the rate of cardiovascular death, myocardial infarction, or stroke, compared with patients treated with the standard drug, clopidogrel (N. Engl. J. Med. 2007;357:2001–15). But because prasugrel treatment was also linked with a 32% relative increase in major bleeding events, compared with clopidogrel, some physicians wondered whether the benefits of prasugrel were worth its increased risk.
“Prasugrel is not a drug for all patients,” Dr. Stephen D. Wiviott said while presenting a poster on the diabetes analysis at the European Society of Cardiology. “Physicians need to weigh things like a patient's age, their bleeding risk, and their risk for ischemic events.”
An increased risk for ischemic events in diabetics is one reason why prasugrel was especially effective for those patients. The combination of higher clinical event rates and a greater relative treatment effect in diabetic patients led to markedly greater absolute event reductions in these patients, compared with those without diabetes, Dr. Wiviott and his associates reported.
The study enrolled 3,146 patients with diabetes and 10,462 patients without diabetes. Among the diabetic patients, 776 (25%) required insulin treatment. The incidence of cardiovascular death, nonfatal MI, or nonfatal stroke (the combined primary end point for the study) was 32% higher among the diabetic patients not taking insulin, compared with the nondiabetics. The event rate was 84% higher in the patients on insulin, compared with the nondiabetic patients.
Patients with unstable angina or ST- elevation myocardial infarction were randomized to treatment with either prasugrel or clopidogrel prior to undergoing percutaneous coronary intervention, and continued on the study medication for a median of 14.5 months, which was also the median time for tallying the incidence of clinical end points. The average age of the patients was 61 years.
In all patients with diabetes, the incidence of the combined primary end point was 12.2% among the patients treated with prasugrel and 17% among those treated with clopidogrel, a 30% relative risk reduction by prasugrel that was statistically significant. (See box.) In contrast, among patients without diabetes, the event rate was 9.2% in patients treated with prasugrel and 10.6% in those treated with clopidogrel, a relative risk reduction by prasugrel of 14% that was still large enough to be statistically significant, reported Dr. Wiviott, a cardiologist at Brigham and Women's Hospital and Harvard University in Boston.
The added benefit from prasugrel, compared with clopidogrel, was even more dramatic in the insulin-requiring diabetics. Within this subgroup of 776 patients, the combined event rate on prasugrel was 14%, compared with 22% in the clopidogrel group, a 37% relative risk reduction. Among the 2,370 patients with diabetes who did not require insulin, prasugrel treatment produced an 11.5% combined event rate and clopidogrel had a 15.3% rate, for a relative risk reduction of 26%.
The extra benefit from prasugrel in patients with diabetes was not associated with an increased risk in major bleeds. In all of the diabetic patients the major bleeding rate was 2.5% with prasugrel and 2.6% with clopidogrel. The excess of major bleeds linked with prasugrel seen in the entire study was entirely driven by the excess in patients without diabetes. In that subgroup, patients on prasugrel had a 2.4% major bleed rate, compared with a 1.6% rate in patients treated with clopidogrel, a relative increased risk of 43% with prasugrel that was statistically significant.
Another prespecified analysis of the study was to evaluate the net clinical benefit of treatment, which was calculated by adding the rate of the composite primary end point and the incidence of major bleeds. In the patients with diabetes, this quadruple tally of adverse events occurred in 15% of the prasugrel-treated patients and 19% of those on clopidogrel, a 26% relative reduction with prasugrel that was statistically significant. In nondiabetic patients, the quadruple composite rate was about 12% in both groups. Prasugrel reduced the risk by a relative 8%, but this difference was not statistically significant.
On the basis of other analyses from the study, prasugrel treatment did not have an advantage over clopidogrel in patients with a history of stroke or a history of bleeding, and in patients aged 75 or older, and so these parameters define patients who are not good candidates for treatment with prasugrel, Dr. Wiviott said in an interview. The results also suggested that the prasugrel dosage used in the study, a 60-mg loading dose followed by a daily 10-mg maintenance dose, probably should be reduced in patients who weigh less than 60 kg.