March 23rd, 2015
Putting PROMISE in Greater Context
Daniel Mark and Larry Husten, PHD
The PROMISE trial, which was presented and discussed in a Journal Club forum at ACC.15, prompted some interesting discussion when CardioExchange covered it as a news story on March 14. Dr. Daniel B. Mark, one of the PROMISE investigators, now sheds further light on the trial in response to questions from CardioExchange news writer Larry Husten.
Click here for CardioExchange’s news coverage of PROMISE and the related discussion.
Click here for a short interview with Dr. Pamela S. Douglas, PROMISE’s lead investigator.
THE INTERVIEW
Husten: Why did the NIH shorten the follow-up period rather than increase it (or stop the trial)?
Mark: I am not in a position to speak for the NIH, nor am I privy to its decision making process. But given the recent budgetary pressures it has faced, I suspect that it is almost never in a position to add funding to an existing trial. At least that has been the feedback I have heard repeatedly from the NIH about multiple large RCTs. Also, it’s worth remembering that many of the primary outcome events were seen in the first year, so this may be a good example of a trial, where longer follow-up does not add treatment related events as efficiently as enrolling more patients who are followed for a shorter period. Given a fixed amount of funds, one has to decide the best way to meet the trial objectives, never a simple decision in an ongoing trial.
Why would they stop the trial? That question suggests that you believe that the only benefit of a trial is to hit the target p value on the primary endpoint. I would not agree with that position at all.
Husten: Given the failure to establish either superiority or noninferiority, how can the trial support a change in guidelines, as Dr. Douglas suggested several times at ACC?
Mark: As we discussed in the Journal Club session at ACC, to formulate a project as a fundable grant to the NIH, it is almost always advisable to pose it as a test of superiority. Noninferiority may work well enough for FDA drug approval, but NIH trials are very different.
That said, proposing a superiority hypothesis does not mean that the expert consensus was that this was likely to be true. It was possibly true, but also possibly not true. What it does is to take a complex question and make it tractable. By specifying a superiority hypothesis with all the associated parameters, we can use the model of Neyman–Pearson hypothesis testing to calculate sample size/power. But most of what goes into that model is a guess. We clothe the process in an aura of scientific rigor, as if that imbues it with some special authority — but in the end it’s mostly educated guesswork. That is not a bad thing; it is the reality of how we figure things out. We currently have no better way to decide how big a trial needs to be.
There are also budgetary constraints. NIH does not have unlimited funds to invest in every RCT, so one has to negotiate a reasonable sample size for a trial based on both a reasonable power story and an acceptable budget. As you know, trials are enormously expensive and we therefore require much more of them than is probably reasonable. That is to say, we expect each trial to definitely settle all our disputes and resolve all our uncertainties — and that simply is not a realistic expectation. Each trial is, in scientific terms, one set of measurements. To really understand something in science, we need to do repeated sets of measurements (multiple trials), but we mostly can afford only the one set. So we try to find clever ways of statistical argument that make it seem as if the one can serve for the many we actually need.
The FDA set up this whole set of fixed rules years ago, in order to operationalize its mandate from the Congress to establish that FDA-approved drugs are safe and effective. Because the FDA rules seemed so rigorous, others started adopting them, and we are now at a place where many clinicians and some statisticians actually think these rules ensure “correct” science. If only it were that simple! The rules are a form of theater. They are probably quite reasonable for FDA decision making, given the pressure cooker of interests that converge on each decision that agency makes. But there is no reason for the rest of us to adopt those rules as gospel, except that it liberates us from the responsibility to think about things more deeply and insightfully — and to exercise judgment. Judgment is an essential part of the scientific process but is often disparaged by those who seek to make science completely objective, above all need for human interpretation.
PROMISE is incredibly valuable because we enrolled the group of patients we wanted, those with about a 50% pretest probability of disease, and got a sample of 10,000 (more than 50% women) with real outcome data, something never before achieved. They are high-quality randomized data from which we can learn much. Yes, some judgment is required to interpret the findings, but that is always the case. Think about what we know now in the context of the anxieties about CTA before the trial was done. If creation of guidelines were simply a matter of applying the fixed rules, perhaps PROMISE would not be so useful.
But that is not the way guidelines are actually written, so it is quite likely, in my view, that the guideline committees will look at these data and alter the recommendations they make around the use of CTA in the context of PROMISE. Guidelines in this area do not state that one test is better than another. How could they? They state that various tests are reasonable to use for a given problem, given the evidence available. But, of course, we have no knowledge of any actual official guideline action or position, so this is simply my opinion.
Husten: Are you concerned that the higher rate of revascularization with CTA did not lead to improved outcomes?
Mark: With respect to extra revascularization procedures, PROMISE was not nearly large enough to detect the effect of this level of shift in revascularization procedures on outcome. Consider that ISCHEMIA is studying revascularization versus optimal medical therapy in a higher-risk population of 7000 patients with moderate or severe ischemia to get at this answer, and it quickly becomes clear that PROMISE cannot answer the question of how these patient outcomes were altered by these incremental procedures. But just as we cannot prove that the patients benefited from the procedures, it would be an error to conclude that the patients did not benefit. It’s like trying to look at a virus with an optical microscope — you just do not have the resolution power to do it. But that does not mean that viruses do not exist.
Husten: Do the findings support a no-imaging/watchful-waiting strategy?
Mark: No imaging/no stress testing was not studied in PROMISE, so the study data do not address that option. Remember that all of these patients went to their doctor with chest pain/dyspnea that the doctor thought could be due to obstructive CAD, and the doctor felt that noninvasive stress testing was indicated to clarify the nature of the patient’s problem. The patients wanted to know if they were ok, and the doctors did not feel comfortable just reassuring them on the basis on an office exam alone.
Husten: If you had known the results of this trial 15 years ago, would we or should we have spent many millions of dollars to make this technology ubiquitous?
Mark: The ability to see clearly inside the body without having to cut patients open is a huge advance in medicine. The 1979 Nobel Prize was awarded for development of CT. It’s clearly worth the money. The question of how to use it wisely is still a work in progress. I believe that PROMISE gets us one big step further along that road. It is also worth noting that the CTA technology is not currently widely reimbursed in the outpatient setting, in large part because of the pre-PROMISE controversies about how this technology would affect practice. The PROMISE data should also provide more comfort on that score.
One final point: It is worth remembering what evidence led us to think that functional stress testing with echo and nuclear methods was the standard for high-quality cardiovascular care. It was primarily sensitivity and specificity data, mostly from different cohorts — that is, echo data in one, nuclear in another. ECG was the only one also measured in each, but the selection biases in creating those stress-imaging cohorts, relative to a standard stress ECG cohort, were mostly ignored by people interested in proving that their technology was better.
JOIN THE DISCUSSION
What’s your take on PROMISE and Dr. Mark’s analysis of it?
March 23rd, 2015
Dangerous Interaction: New Hepatitis C Drug and Old Arrhythmia Drug
Larry Husten, PHD
Late last week Gilead Sciences issued a warning about a rare but potentially fatal interaction between its stellar new hepatitis C drug sofosbuvir and amiodarone, a potent but tricky antiarrhythmic agent. Sofosbuvir is marketed as Sovaldi and, in combination with another antiviral agent, as Harvoni. Amiodarone is a class III antiarrhythmic with a number of different side effects and an extremely long half-life. Its use is generally reserved for difficult cases.
The company reported nine cases of symptomatic bradycardia. One patient died of a cardiac arrest and three patients received a pacemaker. Six cases occurred during the first day of treatment with sofosbuvir. Several patients were taking additional antiviral agents and seven patients were also taking a beta blocker. The company said the mechanism of action for the interaction is unknown.
Paul Sax, an infectious diseases specialist at the Brigham and Women’s Hospital, said that “this is a very uncommon drug-drug interaction. In the short-term, I anticipate it will have almost no effect on prescribing practices.”
A Baird analyst also said it is unlikely that the news will have a significant impact on the use of sofosbuvir. He estimated that there were about 1,000 patients taking amiodarone among the more than 200,000 patients who have received sofosbuvir so far. He noted that the baseline bradycardia risk for amiodarone by itself is about 2.5% per year.
The company said that the co-administration of sofosbuvir and amiodarone is not recommended. In cases where there is no alternative to co-adminstration, Gilead recommends close cardiac monitoring of patients, including monitoring in the hospital for the first 48 hours of treatment.
March 18th, 2015
Networking Opportunities and Cardiology Bootcamp at ACC.15
Saurav Chatterjee, MD
Saurav Chatterjee is a Cardiology fellow blogging this week for CardioExchange in San Diego at this year’s annual ACC conference. For more of our ACC.15 coverage including late-breaking news and in depth analysis, stay tuned to our ACC.15 Headquarters.
As the annual scientific sessions draw to a close, a few of the other ‘small-but-engrossing sessions’ deserve mention.
First of all, a dedicated Fellows-in-Training (FIT) lounge served as a great venue for meeting people, networking, or just plain lounging while grabbing some snacks. The organizing committee deserves special kudos for setting this up. I don’t recall prior iterations of the ACC or other national meetings having a dedicated space for fellows and being successful simultaneously in helping them group together.
A great session of EKG review by the superb Dr. Podrid in the FIT lounge held a relatively modest audience enthralled for two sessions in the afternoons.
Informative networking and ‘meet-the-mentor’ sessions again at the FIT lounge deserve a definite word of acknowledgement.
Finally, as a budding interventional Fellow I was absolutely enthralled by the bootcamp sessions set up by the TCT-ACC-i2 faculty. These were dedicated sessions where some of the most renowned interventionists in the country imparted pearls of wisdom in a case-based format for an audience largely comprised of interventional fellows or young faculty. I hope the other national societies—as well as future ACC meetings—will retain similar flavor and improve on these.
Word of regret: while we as trainees keep hearing that academic medicine is losing attraction and many a devout follower, I personally feel that such bootcamp-like sessions—for grant writing and one-on-one interactions with mentors to provide tips on how to survive and hopefully thrive in academia as Fellows or early career physicians in a busy specialty like cardiology, and many of its sub-specialties—may be successful in retaining at least some of those giving up on pursuit of an academic career.
March 17th, 2015
CABG vs. PCI for Multivessel CAD: Do Second-Generation Stents Make a Difference
wpengine
By Howard C. Herrmann, MD
Second-generation stents narrow the gap between coronary artery bypass grafting and percutaneous coronary intervention for nondiabetic patients with multivessel disease, according to findings from two studies published in the New England Journal of Medicine.
The studies provide a wealth of data informing clinicians and patients about the differences between CABG and PCI for multivessel coronary artery disease. PCI may offer early safety benefits for stroke, bleeding, and potentially mortality, but poses a greater need for repeat revascularization. Later mortality is similar with the two procedures, but MI rates may be higher after PCI. Overall, these data suggest few differences, except for patients with diabetes and for those in whom complete revascularization cannot be attained. This gives the edge to the less invasive approach, which most patients tend to prefer.
The study details:
In a noninferiority study, 880 Asian patients with multivessel disease were randomized to CABG or PCI with everolimus-eluting stents (EESs). At 2 years, the primary endpoint (death, MI, or target-vessel revascularization) was similar in the two groups (PCI, 11%; CABG, 8%), although the difference became statistically significant by 5 years (15% vs. 11%), due primarily to more repeat revascularizations and a trend toward more MIs with PCI. The primary endpoint significantly favored CABG among diabetics, but not among nondiabetics.
In the second study, investigators used registry data to compare outcomes in 9000 multivessel disease patients undergoing PCI with EESs and 9000 undergoing CABG. Early 30-day mortality and stroke were superior with PCI. At 3 years, the groups, including a diabetes subgroup, had similar mortality. Subsequent spontaneous MI was about 1% annually more frequent after PCI than after CABG, but only when revascularization was incomplete.
Dr. Herrmann is deputy editor for NEJM Journal Watch Cardiology, from which this story was adapted.
March 17th, 2015
Vitamin D Supplements Do Not Appear to Lower Blood Pressure
wpengine
By Jenni Whalen
Vitamin D supplements do not effectively lower blood pressure, according to a systematic review and meta-analysis in JAMA Internal Medicine. Low serum vitamin D levels have previously been associated with elevated blood pressure and cardiovascular events.
Researchers examined findings from 46 randomized, placebo-controlled trials that involved at least 4 weeks’ use of vitamin D supplementation (for any indication) and reported both baseline and follow-up data on blood pressure. Individual patient data were also acquired from 27 of those trials (3000 patients).
Within both data sets (trial level and individual patient level), vitamin D supplementation did not significantly affect systolic or diastolic blood pressure. Findings were similar in subgroup analyses limited to patients with elevated baseline blood pressure or diabetes.
“The lack of effect argues against a role for vitamin D supplementation as a means of BP control in individual patients or as a population-based intervention,” the authors conclude.
March 17th, 2015
ACP Recommends Against Screening Asymptomatic Adults for Cardiac Disease
The American College of Physicians has recommended that clinicians should not screen low-risk, asymptomatic adults for heart disease.
In guidelines published in the Annals of Internal Medicine, the ACP says that adults with a 10-year risk for coronary heart disease events under 10% should not undergo screening with resting or stress electrocardiography, stress echocardiography, or stress myocardial perfusion imaging. There is no evidence that these tests improve patient outcomes, but they can lead to increased costs and possible harms, such as radiation exposure and unnecessary follow-up tests.
Instead, clinicians should focus on strategies to modify risk factors — such as smoking, diabetes, hypertension, and hyperlipidemia — and encourage physical activity.
March 16th, 2015
Folic Acid Supplementation Helps Reduce Stroke Risk in Certain Populations
Nicholas Downing, MD
Supplementation with folic acid might help prevent stroke in adults with hypertension — particularly in those with low serum folate levels — according to a study presented on Sunday at the American College of Cardiology conference in San Diego and published in JAMA.
Over 20,000 Chinese adults with hypertension and without histories of MI or stroke were randomized to receive daily enalapril either alone or combined with folic acid (0.8 mg). During roughly 4.5 years’ treatment, first strokes occurred significantly less often with enalapril plus folic acid than with enalapril alone (2.7% vs. 3.4%). The benefit was greatest among participants with the lowest baseline folate levels.
Editorialists note that previous trials showing no benefit of folic acid were conducted in populations with higher baseline folate levels (for example, in the U.S., where grains are fortified with folic acid). They conclude: “This study seems to support fortification programs where feasible, and supplementation should be considered where fortification will take more time to implement.”
March 16th, 2015
Learning Opportunities for Fellows-in-Training at ACC 2015
Saurav Chatterjee, MD
Saurav Chatterjee is a Cardiology fellow blogging this week for CardioExchange in San Diego at this year’s annual ACC conference. For more of our ACC.15 coverage including late-breaking news and in depth analysis, stay tuned to our ACC.15 Headquarters.
There have been a couple of interesting sessions for fellows-in-training and early career professionals amid the ‘buzz’ around the late-breakers and the myriad networking and learning opportunities in beautiful and sunny San Diego.
This year I got a chance to sit in on the Accreditation Compliance Work Group (ACWG) to identify potential areas of concern with the current system of annual disclosures. Some of the problem areas identified included presenters occasionally disregarding relatively small amounts paid, monetary disbursements being made to institutions instead of individuals, conflicts developing in the intervening period between abstract acceptance and actual presentation, and the absence of a framework to systematically identify and potentially take punitive action for non-adherence to current guidelines. There seem to be exciting times ahead for FITs, with training sessions being offered by the ACC to learn more about the process and the opportunity of auditing different presentations at future meetings. Stay tuned!
Also, there is a nice clinical simulation hands-on session on offer at the ACC—great for senior residents and fellows-to-be, or for first-year fellows to hone and refresh clinical knowledge and skills with simulation at booth #3932.
March 16th, 2015
Selections from Richard Lehman’s Literature Review: March 16th
Richard Lehman, BM, BCh, MRCGP
CardioExchange is pleased to reprint this selection from Dr. Richard Lehman’s weekly journal review blog at BMJ.com. Selected summaries are relevant to our audience, but we encourage members to engage with the entire blog.
NEJM 12 March 2015 Vol 372
Endovascular Therapy for Ischemic Stroke with Perfusion-Imaging Selection (pg. 1009): Stroke is a wonderfully straightforward word. When used in a medical context, everybody thinks of a sudden blow. It is something that needs swift action. But actually “stroke” isn’t a straightforward word: ask the cat that has just jumped on to my lap. Now it means a slow and pleasurable process in which she purrs while I pass my hand along her back. That’s the problem with words with deep Indo-European roots: the *streig root is well preserved in several languages, but over thousands of years it has come to mean almost opposite things. And brain strokes can vary between anything from a hammer stroke, which obliterates life, to a brush stroke, which causes some local weakness for a few days. The problem lies between the two ends, and in the need for investigations and treatment to be done at great speed. Two trials of endovascular therapy for ischaemic stroke with perfusion imaging selection in this week’s NEJM present a major advance in stroke treatment, but also illustrate these difficulties. The interventions compared in the first trial (mainly Australian and publicly funded) were intravenous alteplase within 4.5 hours with or without endovascular thrombectomy using the Solitaire FR (Flow Restoration) stent retriever. The patient groups had a mean age of 68 and 70 (the groups were not perfectly matched), and had occlusion of the internal carotid or middle cerebral artery, and evidence of salvageable brain tissue and ischaemic core of less than 70 ml on computed tomographic (CT) perfusion imaging. The trial was stopped prematurely because the thrombectomy group showed markedly better neurological improvement at three days and 90 days.
Randomized Assessment of Rapid Endovascular Treatment of Ischemic Stroke (pg. 1019): The second trial was broadly similar and had a similar outcome: it was stopped early for efficacy. It was funded by Covidien, the manufacturers of the Solitaire FR device, but unlike the publicly funded trial it did not insist on the exclusive use of their product—strange! Anyway, the message is clear. If you have the means to select these patients, by CT angiography and CT perfusion imaging, then they will have a 2.6 fold better chance of a good neurological outcome if treated first with IV alteplase and then with a reperfusion procedure within 60-90 minutes. But pause a minute to consider what this might mean for stroke service provision. Time is of the essence: previous trials of reperfusion, like MR CLEAN, failed because their time frames and selection procedures were looser. So you need very rapid means of transfer and cutting edge CT technology with a team able to interpret it. The team must then discuss their recommendation with the patient or relatives, and proceed at once to perform a quite sophisticated procedure with its own hazards and learning curve. Adoption will not happen at a stroke.
JAMA 10 March 2015 Vol 313
Innovation and Implementation in Cardiovascular Medicine (pg. 1007): “The TAVR [transcatheter aortic valve replacement ] story is a wonderful example of a transformative technology that began with an idea many dismissed, gained momentum through iterative device modifications pioneered by industry, earned an increasing sense of feasibility with animal research and early human studies, achieved US Food and Drug Administration approval after reporting of findings from a pivotal randomized clinical trial, and expanded to additional clinical sites that met quality standards.” In their Viewpoint on Innovation and Implementation in Cardiovascular Medicine, the president of the American College of Cardiology and his colleague cite this “wonderful example” of the American Dream come true, but go on to lament the paucity of other examples. The answer? America needs more young heroes. “Established researchers and institutions need to support and mentor the next generation of innovators. If the courageous pioneers of cardiac surgery did not have the freedom to experiment or the strength to fail 50 or 60 years ago, where would cardiovascular care be today?” I see their point, but cardiovascular care today all too often consists of doing the interventions; plonking in the drugs (regardless of individualised preferences and likelihood of benefit); and a spiral of cost, futility, and repeated admission as the inevitable end approaches. The true heroes, young and old, will be the physicians and researchers who help to meet the difficult and exhausting needs of real people on the way to cardiac death.
Statin Intolerance (pg. 1011): Last year, the statins debate took some strange and personal turns in the UK. The issues were complex and entangled in unhelpful ways, but one fundamental question is that of statin intolerance: why do the findings of clinical trials and clinical experience appear to differ so much? The best way to determine the true prevalence of statin related muscle pains would be through a large series of n-of-one trials with complete blinding and adequate washout periods; but this is never going to be practical. The worst would be to depend on GP record entries and patient discontinuation. There are some in-between possibilities and I look forward to Ben Goldacre’s coming short book on the topic. In the meantime, if you are interested in the issue, look up this quite useful Viewpoint.
Clinical Outcomes at 1 Year Following Transcatheter Aortic Valve Replacement (pg. 1019): So just how wonderful an example of a transformative technology is TAVR (transcatheter aortic valve replacement)? This study looks at 12 182 procedures performed from November 2011 to the end of June 2013 in 299 American hospitals. The sex ratio was equal and the median age was 85. Most of these people would have been expected to die within a year or two, as TAVR is still mostly a last ditch procedure for people too frail to have open replacement. Among the patients who had TAVR, overall mortality was 23.7%, the stroke rate was 4.1% at one year follow-up. So at present we know that TAVR buys time in the very elderly: the other uses mentioned in the Viewpoint still need fuller evaluation. This is not yet the full American Dream.
The BMJ 14 March 2015 Vol 350
The Diagnostic Accuracy of the Natriuretic Peptides in HF: B-type natriuretic peptide (BNP) is the voice of the ventricles. When things are fine, it is heard as a low hum of content, but put the heart under strain and the murmur becomes a growl, and then a shout. All this happens within a few minutes, and dies down within half an hour. If you remember this, you will see why plasma BNP (or NTproBNP) has the diagnostic characteristics that it has. Below a certain level, it rules out “heart failure.” Above a certain level, it indicates that there is a problem, but it doesn’t tell you what it is or how long it has been going on. You can’t tell which ventricle is shouting or why. Used to monitor treatment, BNP fails because there is too much random variability or background noise. This systematic review sets itself the poorly defined task of “assessing the diagnostic accuracy of the natriuretic peptides in heart failure.” This turns out to mean acute heart failure, and sure enough the review concludes that a heart which is not shouting out BNP is not a heart that is failing. Beyond that, don’t trust it. If your patient has chest crackles and a high BNP, that could be heart failure; or it could be a chest infection with a degree of right ventricular overload. I have had quite a long relationship with this peptide, and it’s been a bit of a disappointment.
Drug Disease and Drug-Drug Interactions: “In this review of NICE clinical guidelines, potentially serious drug-drug interactions were relatively common among recommendations for each of three index conditions (type 2 diabetes, heart failure, and depression) and 11 other common conditions.” This is massively important. We are poisoning far too many patients with guideline driven medicine and thoughtless polypharmacy, not helped by computer systems, which cry wolf so often about drug interactions that we have ceased to take any notice.