Interventional Cardiology. Группа авторов

Interventional Cardiology - Группа авторов


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while in a non‐inferiority framework the alternative hypothesis states that the experimental arm is no worse than the control by a pre‐specified margin. The possible interpretation of trial results is predicated on the study design, as shown in Figure 6.3. The choice of superiority as compared to a non‐inferiority design is influenced by a number of factors including cost, existing therapies, and side effect profiles of different treatments. Direct oral anticoagulants (DOACs), for example, require less monitoring than conventional anticoagulation with oral vitamin K antagonists. Demonstration of non‐inferiority, therefore, may provide sufficient evidence to choose a DOAC in place of a vitamin K antagonist, as was shown in the large randomized Rivaroxaban Once Daily Oral Direct Factor Xa Inhibition Compared with Vitamin K Antagonism for Prevention of Stroke and Embolism Trial in Atrial Fibrillation (ROCKET‐AF) trial comparing rivoraxaban to warfarin in patients with atrial fibrillation [8]. In addition, the great efficacy of certain treatments can require prohibitively large and expensive trials designed to show superiority.

Schematic illustration of example of the most common trial type, including superiority and non-inferiority designs.

      Intention to treat, modified intention to treat, and per‐protocol analyses

      Most major trials use analysis by intention to treat whereby all patients are included in their randomized groups, even though they did not all fully comply with the intended treatments. Such an analysis gives an unbiased comparison of the treatment policies as they were delivered in practice, a so‐called pragmatic trial. Per protocol analyses, which exclude any patient when not on randomized treatment, are potentially biased as it could be the sicker patients who opt out. Moreover, many trials reported analyses by modified intention to treat: this method is similar to intention to treat analyses, but allows the exclusion from the analyses of randomized patients for some justified – and possibly prespecified – reasons. For instance, many trials evaluating the safety of novel strategies present the analyses by modified intention to treat. The Apixaban for Reduction in Stroke and Other Thromboembolic Events in Atrial Fibrillation (ARISTOTLE)[9] and the Effective Anticoagulation with Factor Xa Next Generation in Atrial Fibrillation–Thrombolysis in Myocardial Infarction 48 (ENGAGE‐AF 48) trials [10] – that compared apixaban and edoxaban, respectively, to warfarin in patients with atrial fibrillation – included only bleeding events occurred in randomized patients who received at least one dose of the study drug (modified intention to treat population) in their primary safety analysis, and not all randomized patients.

      Bayesian approach

      In this chapter, we have described the fundamentals of the classic frequentist statistics. Over the last few years, several studies have employed the Bayesian approach in the design of randomized clinical trials. Indeed, the US.Food and Drug Administration has recently recognized that Bayesian analyses could enable smaller trials to be conducted without reduction in the validity of the results.

      Conceptually, these approaches are complementary, yet provide distinct interpretations to the underlying hypothesis being tested. The most frequent of these estimates the probability of detecting a difference as large or larger than what was observed under the assumption of the null hypothesis. This is not immediately intuitive, while the Bayesian approach provides a probability estimate for the alternative hypothesis being true. Anytime a frequentist approach is used, it is necessary to take repeated experiments into consideration: in 95% of these experiments, the observed results will be in the range expressed by the confidence interval. Conversely, Bayesian statistics is strictly connected with conditional probability: Bayes’ theorem says that we can set up a prior information – based on our knowledge – and then calculate posterior probabilities of this prior information. These prior probabilities are updated through an iterative process of data collection. Moreover, they should incorporate information from all relevant research before we perform the new experiment. Of note, as aforementioned, the frequentist statistical approach uses results from completed studies to design a new study but does not formally incorporate these data in the evaluation of the new study hypotheses. Unlike the frequentist approach, Bayesian methods allow prior information to be synthesized with new data.

Schematic illustration of graphic explanation of the results from the SURTAVI trial, reporting posterior probability distribution for the difference in the primary end point.

      These models must recognize the uncertainty in the prior information and that differences might exist between posterior and prior evidence. Indeed, the most important limitation of this approach is that if the prior is wrong, all the following steps of the inductive process will be wrong.

      Reporting of trial findings in medical journals, at conference presentations, and to regulatory authorities need to be of the highest standards whereby an unbiased and detailed report of all relevant findings is presented.

      The objectives, methods, discussion, and conclusions need to be clearly presented in a balanced report. In particular, results and interpretations should include any safety issues (adverse events) as well as efficacy findings. For publications in medical journals, the CONSORT guidelines are helpful to authors, editors, referees, and readers in enhancing the quality assessment of any trial report.

       Interactive multiple choice questions are available for this chapter on www.wiley.com/go/dangas/cardiology

      References

      1 1 Urban P, Meredith IT, Abizaid A, et al. Polymer‐free Drug‐Coated Coronary Stents in Patients at High Bleeding Risk. N. Engl. J. Med. 2015, 373 (21), 2038–47.

      2 2 Le May M, Wells G, So D, et al. Safety and Efficacy of Femoral Access


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