Design Issues of Randomized Phase II Trials and a Proposal for Phase II Screening Trials

Rubinstein, Larry; Korn, Edward L.; Freidlin, Boris; Hunsberger, Sally; Ivy, S. Percy; Smith, Malcolm A.

doi:10.1200/jco.2005.01.149

Cited by 352 publications

(232 citation statements)

References 31 publications

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“…By contrast, we used a clinical outcome for three reasons: the National Institutes of Health want to focus on relapses as a basis for powering a future phase 3 trial, pregnancy decreases relapses, 2 and a small phase 2 trial with monthly MRI scans has already been done. 7 Because this trial was phase 2, we used a signifi cance level of α=0·10 for all analyses, as has been used in cancer trials 27 and in phase 2 trials of stroke, 28 amyotrophic lateral sclerosis, 29 and Parkinson's disease. 30 The use of p<0·10 as signifi cant in phase 2 trials was considered stringent enough to assess the potential for clinical effi cacy of a new intervention, while controlling for false positives and avoiding the much higher costs of the larger sample sizes needed to achieve a p value of less than 0·05.…”

Section: Discussionmentioning

confidence: 99%

“…30 The use of p<0·10 as signifi cant in phase 2 trials was considered stringent enough to assess the potential for clinical effi cacy of a new intervention, while controlling for false positives and avoiding the much higher costs of the larger sample sizes needed to achieve a p value of less than 0·05. 27,28 For the analysis of time to fi rst relapse, we used Kaplan-Meier analysis and log-rank tests to estimate and compare the proportion of patients with fi rst relapse at each timepoint. We used a Cox proportional hazards model to compare the proportion of patients with relapse at 12 months and 24 months, adjusting for age, baseline EDSS score (<2 vs ≥2), number of relapses in the 12 months before the study (≤1 vs >1), duration of multiple sclerosis (<1 vs ≥1 year), previous glatiramer acetate treatment (never vs past or current), and previous interferon treatment (yes vs no).…”

Section: Discussionmentioning

confidence: 99%

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Estriol combined with glatiramer acetate for women with relapsing-remitting multiple sclerosis: a randomised, placebo-controlled, phase 2 trial

Voskuhl

Wang

et al. 2016

The Lancet Neurology

166

143

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SummaryBackground Relapses of multiple sclerosis decrease during pregnancy, when the hormone estriol is increased. Estriol treatment is anti-infl ammatory and neuroprotective in preclinical studies. In a small single-arm study of people with multiple sclerosis estriol reduced gadolinium-enhancing lesions and was favourably immunomodulatory. We assessed whether estriol treatment reduces multiple sclerosis relapses in women.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Estriol combined with glatiramer acetate for women with relapsing-remitting multiple sclerosis: a randomised, placebo-controlled, phase 2 trial

Voskuhl

Wang

et al. 2016

The Lancet Neurology

166

143

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“…15 This is often done if there is limited historical control data or if other treatment factors, such as dramatic changes in supportive care, reduce the applicability of historical controls. 17,18 However, unlike randomized phase 3 trials, these studies are not powered to determine true clinical improvement of the experimental therapy compared to the control arm. 19 Instead, they reinforce that the experimental therapy is potentially efficacious and warrants further study in a larger, appropriately powered phase 3 clinical trial.…”

Section: Multi-stage Phase 2 Trial Designmentioning

confidence: 99%

“…This allows patient data from the phase 2 portion to be included in the final analysis, which dramatically shortens the time to study completion and decreases the number of required patients. 18 However, it does necessitate a pre-study commitment of both time and resources for design and study completion for both the phase 2 and phase 3 portions. Table 1 highlights the important factors required to assess the strength of a phase 2 study.…”

Section: Phase 2/3 Trial Designmentioning

confidence: 99%

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Are There Circumstances in Which Phase 2 Study Results Should Be Practice-Changing?

Tomblyn

Rizzo

2007

Hematology

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New pharmaceuticals, innovative combinations of approved agents, and novel treatment modalities have resulted in a marked increase in the need for clinical trials. Evidence for treatment efficacy is best derived from large phase 3 randomized, controlled clinical trials. However, phase 3 investigations are lengthy and expensive, and consume patient resources. Furthermore, some diseases and treatment indications are rare, and adequate numbers of patients for a definitive phase 3 trial do not exist. Consequently, it is imperative for clinicians to understand phase 2 trial design, since their interpretation is required to apply the findings in clinical practice appropriately. The complexity of phase 2 studies is explored, including unique designs, possible use of randomization, and other key elements necessary for interpretation of phase 2 trials. Specific examples and application of these concepts are discussed in this review.

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Efficacy and Safety of Revacept, a Novel Lesion-Directed Competitive Antagonist to Platelet Glycoprotein VI, in Patients Undergoing Elective Percutaneous Coronary Intervention for Stable Ischemic Heart Disease

et al. 2021

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IMPORTANCEThe assessment of new antithrombotic agents with a favorable safety profile is clinically relevant. OBJECTIVE To test the efficacy and safety of revacept, a novel, lesion-directed antithrombotic drug, acting as a competitive antagonist to platelet glycoprotein VI. DESIGN, SETTING, AND PARTICIPANTSA phase 2 randomized clinical trial; patients were enrolled from 9 centers in Germany from November 20, 2017, to February 27, 2020; follow-up ended on March 27, 2020. The study included patients with stable ischemic heart disease (SIHD) undergoing elective percutaneous coronary intervention (PCI).INTERVENTIONS Single intravenous infusion of revacept, 160 mg, revacept, 80 mg, or placebo prior to the start of PCI on top of standard antithrombotic therapy. MAIN OUTCOMES AND MEASURESThe primary end point was the composite of death or myocardial injury, defined as an increase in high-sensitivity cardiac troponin to at least 5 times the upper limit of normal within 48 hours from randomization. The safety end point was bleeding type 2 to 5 according to the Bleeding Academic Research Consortium criteria at 30 days. RESULTSOf 334 participants (median age, 67.4 years; interquartile range, 60-75.1 years; 253 men [75.7%]; and 330 White participants [98.8%]), 120 were allocated to receive the 160-mg dose of revacept, 121 were allocated to receive the 80-mg dose, and 93 received placebo. The primary end point showed no significant differences between the revacept and placebo groups: 24.4%, 25.0%, and 23.3% in the revacept, 160 mg, revacept, 80 mg, and placebo groups, respectively (P = .98). The high dose of revacept was associated with a small but significant reduction of high-concentration collagen-induced platelet aggregation, with a median 26.5 AU × min (interquartile range, 0.5-62.2 AU × min) in the revacept, 160 mg, group; 43.5 AU × min (interquartile range, 22.8-99.5 AU × min) in the revacept, 80 mg, group; and 41.0 AU × min (interquartile range, 31.2-101.0 AU × min) in the placebo group (P = .02), while adenosine 5′-diphosphate-induced aggregation was not affected. Revacept did not increase Bleeding Academic Research Consortium type 2 or higher bleeding at 30 days compared with placebo: 5.0%, 5.9%, and 8.6% in the revacept, 160 mg, revacept, 80 mg, and placebo groups, respectively (P = .36). CONCLUSIONS AND RELEVANCERevacept did not reduce myocardial injury in patients with stable ischemic heart disease undergoing percutaneous coronary intervention. There were few bleeding events and no significant differences between treatment arms.

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Design Issues of Randomized Phase II Trials and a Proposal for Phase II Screening Trials

Cited by 352 publications

References 31 publications

Estriol combined with glatiramer acetate for women with relapsing-remitting multiple sclerosis: a randomised, placebo-controlled, phase 2 trial

Estriol combined with glatiramer acetate for women with relapsing-remitting multiple sclerosis: a randomised, placebo-controlled, phase 2 trial

Are There Circumstances in Which Phase 2 Study Results Should Be Practice-Changing?

Efficacy and Safety of Revacept, a Novel Lesion-Directed Competitive Antagonist to Platelet Glycoprotein VI, in Patients Undergoing Elective Percutaneous Coronary Intervention for Stable Ischemic Heart Disease

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