The novel, orally administered calcitonin gene-related peptide (CGRP) receptor antagonist, MK-0974, was effective and generally well tolerated for the acute treatment of migraine.
This study confirmed previous findings that telcagepant 300 mg was effective at relieving pain and other migraine symptoms at 2 hours and providing sustained pain freedom up to 24 hours. In this study, telcagepant 150 mg was also effective. Telcagepant was generally well tolerated.
This study provides Class II evidence that in patients with migraine, telcagepant taken daily reduces headache days by 1.4 days per month compared to placebo and causes 2.5% of patients to have elevations of serum ALT levels.
Repeated significance testing in a sequential experiment not only increases the overall type I error rate of the false positive conclusion but also causes biases in estimating the unknown parameter. In general, the test statistics in a sequential trial can be properly approximated by a Brownian motion with a drift parameter at interim looks. The unadjusted maximum likelihood estimator can be potentially very biased due to the possible early stopping rule at any interim. In this paper, we investigate the conditional and marginal biases with focus on the conditional one upon the stopping time in estimating the Brownian motion drift parameter. It is found that the conditional bias may be very serious for existing point estimation methods, even if the unconditional bias is satisfactory. New conditional estimators are thus proposed, which can significantly reduce the conditional bias from unconditional estimators. The results of Monte-Carlo studies show that the proposed estimators can provide a much smaller conditional bias and MSE than the naive MLE and a Whitebead's bias reduced estimator.
The study was underpowered due to enrollment difficulties and did not demonstrate a significant efficacy difference between telcagepant and placebo for the treatment of a migraine attack in patients with stable coronary artery disease. Telcagepant was generally well tolerated for acute intermittent migraine treatment in these patients.
Rizatriptan 10-mg ODT was superior to placebo at providing two-hour pain relief and two-hour pain freedom in the treatment of acute migraine in those who do not respond to sumatriptan 100 mg. Rizatriptan was generally well tolerated in this population.
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