Just as dinosaurs ruled the earth for millions of years, for more than 30 years now cardiology has been ruled by mega-trials. Over the years, the cardiology landscape would shake and tremble as ever more gigantic mega-trials emerged to dominate the field.
Just as the giant dinosaurs paid no attention to the seemingly inconsequential little furry mammals running around beneath their feet, cardiology has tended to ignore or downplay smaller trials -- what I will here call mini-trials.
Consider the reflexive dismissal or diminution of . Critics, many of them proponents and leaders of mega-trials, immediately opined that ORBITA need not be taken seriously, that it could not possibly raise serious questions about current practices and beliefs, because it "only" enrolled 200 patients and "only" followed them for 6 weeks. But these critics never explained why a trial designed to study whether patients with stable ischemic heart disease experience symptomatic relief from PCI would actually need more patients or longer follow-up. For most critics, there was just the blind assumption that bigger is not only better but also necessary. In fact, in this case, bigger could well have been worse, since it could well have produced a statistically-significant difference that in clinical terms would have been meaningless. (This should not be a new concept to anyone who has been paying attention.)
It's not yet widely known that the same group, led by principal investigator Darrel Francis (Imperial College London), is now performing an even smaller trial that could have an equal or even greater impact than ORBITA.
Although it will only enroll 50 patients, an astonishingly small number in a universe dominated by mega-trials, (Self-Assessment Method for Statin Side-effects Or Nocebo) is designed to help solve one of the most pressing, recalcitrant, and annoying problems in all of cardiovascular and preventive medicine: patient resistance to statins.
Statins, of course, have their critics, but most knowledgeable observers have been persuaded by the clinical trial evidence demonstrating their benefits, at least in a very high-risk population of people. The problem is that a large and growing number of people and even many healthcare professionals, including some cardiologists, believe that statins cause all sorts of side effects. Muscle weakness is the most commonly-cited side effect, but there are a litany of others, such as cognitive impairment, that can be terrifying to many potential statin takers.
A few years ago, a group of leading mega-trialists published an enormous that included data from 175,000 randomized patients. They concluded that the evidence supporting both the benefits and safety of statins was overwhelming. The authors were dismayed when their shock and awe strategy did not provoke an immediate retreat or surrender by the anti-statinista forces.
A major limitation of the paper is that the trials included in the meta-analysis did not assess side effects in a uniform or rigorous fashion. Another area of concern is that the patient-level data from the trials has not been made available for outside scrutiny.
But even if we accept the conclusions of the meta-analysis authors and we believe that the true incidence of statin side effects is quite small, we are left with a remaining and quite difficult problem. How does an individual person know whether or not he or she is one of those very few people who have real side effects? This is an inevitable limitation of mega-trials, which study large populations. Patients, however, want to know what it means for them.
SAMSON does something that mega-trials are unable to do. It delivers -- even before the trial is completely finished! -- specific, valuable, and actionable information to the trial participants.
The trial design is remarkably simple and clever. The study population includes adults who have stopped taking statins because of side effects. At the start of the trial participants receive 12 bottles, one for each month, which they take in a predefined random order. Four bottles contain a daily statin (atorvastatin [Lipitor]), four contain a daily placebo, and four are empty. Participants record their symptoms every day in a smartphone app. In addition to the aggregate data from all the trial participants, individual participants will serve as both their own blinded placebo control and unblinded no-treatment control, because four of the bottles are empty.
Although the trial will only enroll 50 patients it should be powerful enough to help answer both the question of the true rate of statin side effects and, even more importantly, at least for the individual participants, whether their own symptoms are caused by statins. Participants will receive their own results at the end of the 12 months -- even before the remaining patients have completed the trial. Thus they should have conclusive information about their own individual side effects. (Of course, we have no way of knowing at this point how that knowledge will be utilized, but at least there will be no question of how the data applies to the individual patient.)
I am not going to argue that mega-trials have no value. Of course they do. But it is should also be clear to all that mega-trials have become increasingly difficult and expensive to perform and that they are often no longer as impactful or interesting as they once were. Too often enormous resources have been devoted to answering questions that industry wants answered instead of being used to answer questions of fundamental importance.
By contrast, small studies like ORBITA and SAMSON demonstrate that, by thinking outside the box, it is still possible to perform original and important research without huge resources. Unless we want the cardiology field to serve as the research arm for industry or Wall Street, we need to encourage and welcome original mini-trials trials like ORBITA and SAMSON that challenge the dinosaurs of our time.