We have read with great interest the article written by Jolicoer et al. (1) about the concordant domain analysis, a new method to interpret early phase trials and we applaud their initiative which expands the horizons in the current context of progressive diffuculties to ran studies.
Randomized controlled trials (RCT) and meta-analysis constitute the highest level of evidence and the chances to succeed are high when there is a strong financial support to launch projects as Further Cardiovascular Outcomes Research with PCSK9 Inhibition in Subjects with Elevated Risk (FOURIER) with 27,564 patients, which in addition to demonstrate the hypothesis of the study, it ensures the external validity and the study of subgroups.
However, recently we are witnessing a progressively more tortuous environment to launch adequately powered RCTs due to economic restrictions, lower margin to demonstrate cost-effectivity of the new treatments and more strict legal requirements and as the authors quote, only 1 in 10 investigational agents tested in phase III trials reaches the market. Some authors have already raisen concerns about the future of research and the protagonism of new methods as adaptive studies(2) or approaches to emulate RCT (3) are foreseen in the near future.
In our opinion, the combination of pilot randomized studies with new iniciatives as the described by Jolicoer may be a promising pathway when the conditions to launch large RCTs are not possible and in fact, we have recently seen examples of small pilot randomized trials with clinical endpoints published in journals of very high impact factor(4). In this way, our group has recently received financial support from a large company of devices to run a pilot study with 400 patients to explore a research question that requires a large and expensive trial of 2000 patients (ANGiographic Evaluation of Left main coronary INtErvention, ANGELINE, NCT04604197).
In summary, we are assisting to relevant changes in the field of research and although RCTs and meta-analysis will be and will have to be always the first goal, new initiatives as the one that Jolicoer et al. share with us deserve our attention and are very welcome.

REFERENCES
1. Jolicoeur EM, Verheye S, Henry TD et al. A novel method to interpret early phase trials shows how the narrowing of the coronary sinus concordantly improves symptoms, functional status and quality of life in refractory angina. Heart 2021;107:41-46.
2. Rapezzi C, Maggioni AP, Ferrari R. Adapting to survive. Eur Heart J 2020;41:3981-3983.
3. Franklin JM, Patorno E, Desai RJ et al. Emulating Randomized Clinical Trials with Nonrandomized Real-World Evidence Studies: First Results from the RCT DUPLICATE Initiative. Circulation 2020.
4. Yannopoulos D, Bartos J, Raveendran G et al. Advanced reperfusion strategies for patients with out-of-hospital cardiac arrest and refractory ventricular fibrillation (ARREST): a phase 2, single centre, open-label, randomised controlled trial. Lancet 2020;396:1807-1816.

The soul-searching analysis by Daniel McKenzie deals with the scenario where both the doctor and the patient recognise that something went wrong(1). The dynamics are different when it is only with the benefit of hindsight that it is only the professionals who realise that, all along, they have been inflicting iatrogenic harm on their patients. Even in that scenario what matters is "What will be done to prevent someone else being harmed in the future?".
The thrombolytic treatment of ST elevation myocardial infarction(STEMI) is a case in point. That treatment strategy was initiated in 1986, and it soon became the standard of care for STEMI(2). Further down the line, in September 2020, a literature review identified 138 cases(with accompanying case histories) of dissecting aortic aneurysm(DAA) characterised by STEMI-like ST segment elevation. These cases were published during the period January 2000 to March 2020(3). Arguably, there must have been, at least, the same number of cases of STEMI-like DAA in the 20 year period following the introduction of thrombolytic treatment of ST elevation myocardial infarction. At the very least, some of those cases must have been harmed by thrombolytic treatment.
Why does that matter in September 2020? It matters because thrombolysis is "back on the agenda" for some myocardial infarction patients with ST segment elevation(4). All this, without the precaution to rule out DAA either by point-of-care transthoracic echocardiography(TTE) or by transoesophageal echocardiography(TOE). The former is non-invasive but suboptimally sensitive, the latter is invasive but much more sensitive.. To mitigate the suboptimal sensitivity of TTE one strategy would be to maximise the pretest probability of DAA by compiling a risk score which encompasses history of backache(which does not need to have a "rearing" quality), documentation of interarm blood pressure difference, presence of the murmur of aortic regurgitation(optimally detected by the Vivid-7 system; GE Medical, Milwauwkee, Wisconsin, USA)(5), focal neurological symptoms and signs, and mediastinal widening on chest radiography. A high pre-test probability of DAA would be sufficient to invalidate a TTE which had failed to detect stigmata of DAA.
Our patients are not aware of the dynamics that come into play when they present with chest pain and a STEMI-like electrocardiogram. They take everything on trust. It would be unconscionable for us to knowingly put them in the way of iatrogenic harm by not heeding the lessons that can be gleaned from the literature on STEMI-like DAA.

I have no funding, and no conflict of interest.
References
(1) McKenzie D
What to do when things go wrong
Heart 2020;doi.org/10.1136/heartjnl 2020.316539
(2) Van de Werf
The history of coronary reperfusion
Eur Heart J 2014;35:2510-2515
(3) Jolobe OMP
Clinical characteristics in STEMI-like aortic dissection versus STEMI-like pulmonary embolism
Archives of Vascular Medicine 2020;4:019-130
DOI:29328/journal.avm.1001013
(4) Vallabhajosyula S., Verghese D., Subramanian AV et al
Management and outcome of uncomplicated ST segment elevation myocardial infarction patients transferred after fibrinolytic treatment
Int J Cardiol IJCA-28800(Article in Press)
(5)Draper J., Subbiah S., Bailey R., Chambers J
Murmur clinic. Validation of a new model for detecting heart valve disease
Heart 2019;105;56-59

Biphasic ventilation for failing Fontan physiology

Seigo Okada1, MD, PhD, Jun Muneuchi1, MD, PhD, Mamie Watanabe1, MD

1Department of Pediatrics, Japan Community Healthcare Organization, Kyushu Hospital, 1-8-1, Kishinuora, Yahatanishiku, Kitakyushu, Fukuoka, 806-8501, Japan

Address correspondence and reprint requests to: Seigo Okada, M.D., Ph.D.
Department of Pediatrics, Japan Community Healthcare Organization, Kyushu Hospital, 1-8-1, Kishinoura, Yahatanishiku, Kitakyushu, Fukuoka, 806-8501, Japan. Tel: 81-93-641-5111; Fax: 81-93-642-1868; E-mail: sokada0901@gmail.com; ORCID: 0000-0002-9150-1913

Dear Editor:
We read the article by Charla et al.1 with great interest. The authors conducted a phase-contrast magnetic resonance study during biphasic ventilation (BPV) in 10 patients aged 20–34 years who had Fontan circulation and 10 matched control subjects. BPV resulted in significant pulmonary blood flow and cardiac output augmentations in the Fontan group, which suggests the importance of “thoracic pump” in Fontan patients without a subpulmonary ventricle. We appreciate the authors’ efforts to assess the efficacy and feasibility of noninvasive external ventilation for Fontan patients. This is a thoughtfully conducted study, but some issues must be further discussed.
First, the authors mentioned that the study was the first to describe the impact of BPV in the Fontan population. However, we previously described the efficacy of BPV for failing Fontan circulation in a 16-year-old male patient with hypoplastic left heart syndrome who presented protein-losing enteropathy and plastic bronchitis (PB).2 He underwent rehabilitation using an RTX respirator (Medivent Ltd., London, UK) with the vibration mode set at −10/+10 cm H2O for 3 minutes, followed by the cough mode set at −9/+18 for 1 minute, three times for 12 minutes per session.3 The brief period of BPV increased the stroke volume without changing the heart rate. After the start of the BPV, the PB, hypoalbuminemia, and congestive symptoms all improved. No signs of recurrent circulatory failure have since been observed. As the management strategy for the complex pathophysiology of Fontan circulation is not yet established, their and our results suggest that BPV can be an effective treatment and preventive rehabilitation for failing Fontan circulation.
Second, several Fontan patients were likely to have no significant pulmonary blood flow and cardiac output augmentations during BPV.1 In the practical setting of BPV, it is important for a cuirass to fit the patient’s chest. Thereby, we wonder whether overweight or obesity is a risk factor of ineffective BPV. Do you have data regarding the relationship between body mass index and augmentation of pulmonary blood flow during BPV in your cohort? Pulmonary arterial size is an important determinant of pulmonary circulation in Fontan patients. A recent report has shown that pulmonary arterial size expressed as Nakata index is an independent predictor of functional clinical status in adult Fontan patients.4 Thus the relationship between pulmonary arterial size and augmentation of pulmonary blood flow during BPV should also be addressed.

1. Charla P, Karur GR, Yamamura K, et al. Augmentation of pulmonary blood flow and cardiac output by non-invasive external ventilation late after Fontan palliation. Heart Published Online First: 06 July 2020. doi: 10.1136/heartjnl-2020-316613
2. Okada S, Muneuchi J, Nagatomo Y, et al. Successful Treatment of Protein-Losing Enteropathy and Plastic Bronchitis by Biphasic Cuirass Ventilation in a Patient with Failing Fontan Circulation. Int Heart J 2018;59:873-6.
3. Pediheart Podcast 49: Surveillance of the Fontan Patient + Novel Ventilation Approaches for the Fontan Patient. Available from: https://podcasts.apple.com/us/podcast/pediheart-podcast-49-surveillance-... (accessed July 18, 2020).
4. Ridderbos FS, Bonenkamp BE, Meyer SL, et al. Pulmonary artery size is associated with functional clinical status in the Fontan circulation. Heart 2020;106:233-9.

The benefits of regular exercise are non deniable with reduction in all cause, cardiovascular and cancer mortality (1,2,3). Endurance exercise with increase in cardiac output results in dilatation of left ventricular cavity size and eccentric hypertrophy with low normal ejection fraction that is a dilated cardiomyopathy phenocopy. The ability to distinguish true pathology from physiological remodelling remains a difficult area for cardiologists. Frequently asymptomatic athletic individuals are referred to the cardiology service with abnormal resting 12 lead ECGs. They must be appropriately investigated. The dimema for the investigating cardiologist is to determine the healthy athlete from the athlete with DCM. An erroneous diagnosis of DCM in an athlete may lead to unnecessary disqualification from sport, unnecessary pharmacotherapy and a decline in physical and psychological well being as well as implications for life insurance. Millar et al study adds vital information to the field (4). It is reassuring that the study reported that none of the athletes with a physiologically increased LV size and borderline or low resting LV ejection fraction (grey-zone participants) had replacement fibrosis of the left ventricular myocardium on cardiac MRI. In addition, the authors have reported that functional assessment of the heart by stress echocardiography can discriminate between DCM and DCM phenocopy with high sensitivity and specificity. This study will likely be a game changer in the investigation of athletic remodelling and may reduce the requirement to ask athletic individuals to decondition and refrain from their sport.

1. Parry-Williams, G., Sharma, S. The effects of endurance exercise on the heart: panacea or poison?. Nat Rev Cardiol 17, 402–412 (2020).
2. Fiuza-Luces, C. et al. Exercise benefits in cardiovascular disease: beyond attenuation of traditional risk factors. Nat. Rev. Cardiol. 15, 731–743 (2018).
3. Pedisic, Z. et al. Is running associated with a lower risk of all-cause, cardiovascular and cancer mortality, and is the more the better? A systematic review and meta-analysis. Br. J. Sports Med.
4.Millar LM, Fanton Z, Finocchiaro G, et al Differentiation between athlete’s heart and dilated cardiomyopathy in athletic individuals Heart 2020;106:1059-1065.