INCLUSION/EXCLUSION CRITERIA 1. The following are considerations when defining the cardiac arrest trial patient population (i.e., the inclusion/exclusion.

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Presentation transcript:

INCLUSION/EXCLUSION CRITERIA 1. The following are considerations when defining the cardiac arrest trial patient population (i.e., the inclusion/exclusion criteria): The defined trial population can support a reasonable enrollment rate; The defined trial population can support a reasonable enrollment rate; The population defined has the potential for providing scientifically valid data; The population defined has the potential for providing scientifically valid data;1

INCLUSION/EXCLUSION CRITERIA The population defined (and thus the results obtained from these patients) may be able to support a wider population of cardiac arrest patients.The population defined (and thus the results obtained from these patients) may be able to support a wider population of cardiac arrest patients.2

INCLUSION/EXCLUSION CRITERIA a.Should the study exclude non-witnessed arrests, or should the study include both witnessed as well as non-witnessed arrests? b. Should the study only include those patients with documented ventricular fibrillation? c.Based on the literature regarding early intervention and survival outcomes, should there be a limit on the time that has elapsed between arrest and initiation of CPR? If so, can you suggest how best to obtain accurate, unbiased time estimates? 3

INCLUSION/EXCLUSION CRITERIA d.Should the study patients be limited to patients who have arrested in the field, or should the study also include in-hospital cardiac arrest patients ? e. If field patients are to be included, should CPR be initiated by professionals only, or can patients be enrolled if timing is recorded by, and CPR is initiated by bystanders? f. Do you have any other suggestions regarding the inclusion/exclusion criteria? 4

STUDY ENDPOINTS 2. What would appropriate clinical endpoints be for efficacy in a cardiac arrest study? a.Survival? If so, how would “survival” be defined? E.g., Would functioning in a vegetative state be considered “surviving”? b.Neurological/neurocognitive? What are meaningful neurological endpoints and how should they be evaluated? Is a composite endpoint acceptable? 5

STUDY ENDPOINTS c.Are there clinically acceptable surrogate endpoints that can be used? E.g., Return of spontaneous circulation, 24 hour survival, hemodynamic improvement, quality of life, work status/functional status, etc. Should these surrogates be primary or secondary endpoints? 6

STUDY ENDPOINTS 3. Based on the clinical endpoints discussed above, what length of follow-up should be considered for the efficacy endpoints? E.g., If a device was associated with a 24 hour survival advantage but did not improve hospital mortality, would this device be considered efficacious? 4. What should the primary composite safety endpoint include? 7

STUDY ENDPOINTS 5. What length of follow-up should be considered for the safety endpoint? 8

STUDY DESIGN 6. Can a scientific study be performed using a single arm study with historical controls (US and/or OUS)? If so, should the historical controls meet the same inclusion/exclusion criteria? Do you have any suggestions on how to reduce bias if historical controls and/or OUS data are used? 9

STUDY DESIGN 7. If the study is unblinded, do you expect any substantial positive or negative placebo effect, or an effect of investigator bias on patient selection or endpoint evaluation? If so, how can these problems be minimized? 10

STUDY DESIGN 8. Should the trial design be a non-inferiority (i.e., equivalence) or superiority study for safety and efficacy? a.Under what conditions could an equivalence trial be acceptable? E.g., limited labeling/claims? b.If non-inferiority, what equivalence delta(s) would be clinically acceptable for the safety and effectiveness endpoints discussed above? 11

STUDY DESIGN c. If superiority (i.e., new technology would need to demonstrate improvement over current technology), are there new clinical trial designs that can be considered, e.g., superiority for surrogate endpoint and equivalent hospital discharge rates; or additional post-market studies on devices/technologies to supplement initial pre-market approval safety/effectiveness data. 12

STUDY DESIGN 9. Discuss the possibility of developing a registry and using the data for future studies. What are some of the necessary data points that should be collected, keeping in mind the use of this data as historical controls for future studies. 13

ADVERSE EVENTS 10 Can uniform definitions of adverse events be created? If yes, by whom? 14