Recent eLetters

We read with interest Dr Tayler et al's piece entitled 'Diagnosing an MI: don't trust the monitor!'[1]. We have had a similar experience with ECG filter-related artefactual ST segment change, resulting in patient referral direct to the catheter lab for primary percutaneous coronary intervention. As a consequence, we have audited the variation in ECG filter settings utilised during the acute coronary syndrome 'patient journey'. We found that patients (n=50) had ECGs acquired using up-to 4 different (average 2.14 /-0.99) filter settings during their admission. Across the hospital trust, 15 different filter settings were in operation and only 10% of ECGs met the AHA standard of 0.05-100Hz[2]. Our audit findings have increased awareness of the importance of ECG filter settings in the fidelity of ECG recording and led to standardisation of all ECG equipment in the trust, hopefully limiting the inappropriate diagnosis of ST segment elevation. We congratulate the authors on raising awareness of this problem and encourage others to review the set-up of their ECG equipment

1. Tayler, D., J. Gunn, and D. Chamberlain, Diagnosing an MI: don't trust the monitor! Heart. 96(5): p. 408-408. 2. Bailey, J., et al., Recommendations for standardization and specifications in automated electrocardiography: bandwidth and digital signal processing. A report for health professionals by an ad hoc writing group of the Committee on Electrocardiography and Cardiac Electrophysiology of the Council on Clinical Cardiology, American Heart Association. Circulation, 1990. 81(2): p. 730-739.

Conflict of Interest:

None declared

Trans-radial procedures â₉€œ still two weights and two measures? (letter regarding article from SL Hetherington, Heart 2009;95:1612-1618)

Bernardo Cortese, MD ª Cardiologia Interventistica, Fondazione IRCCS Caâ₉„¢ Granda Ospedale Maggiore Policlinico, Milano, Italy

We read with great interest the article from SL Hetherington et al. regarding the impact of trans-radial primary PCI on clinical outcome in a single-center experience.[1] Authors discovered lower (although not statistically significant) in-hospital mortality rates and lower major cardiac or cerebrovascular adverse events with this technique, compared to the standard trans-femoral route. Previous studies regarding this topic were small, single-centre experiences, therefore not powered enough to demonstrate a significant clinical impact of the trans-radial technique during urgent PCI. Today, this study covers a vacuum in the literature, and being us â₁“radialistsâ€� since our very first PCI, we appreciate that.

Anyhow, despite the well-known lower hospital stay and costs, and now with the help of such clinical evidence, Authors and the community of interventional cardiologists should now investigate why this technique is still so underused in western countries. We wonder why if a single centre uncontrolled clinical trial is able to change the overall acute myocardial infarction management in the cath lab,[2] multi-centre, multi-national, old and recent [1, and Schäufele TG, in http://directnews.americanheart.org/extras/sessions2009/slides/41_pslides.pdf, accessed 29 Nov 2009] clinical evidence-based and economical evidence-based medicine should not change current practice.

The extent of the problem of â₁“radial resistanceâ€� may be easily understood given the following numbers. Until a few years ago, only 30% of European centres adopted a routine trans-radial approach for PCIs.[3] And has been recently disclosed that in only 1.32% of overall procedures performed in the US such approach is used.[4]

We believe that the interventional community should stop seeing at radialists as weird colleagues and start to change their mind. Now it is not time to call for a randomized trial. This is time to call for awareness.

[1] Hetherington SL, Adam Z, Morley R, et al. Acute coronary syndromes: Primary percutaneous coronary intervention for acute ST-segment elevation myocardial infarction: changing patterns of vascular access, radial versus femoral artery. Heart 2009;95:1612-1618. [2] Vlaar PJ, Svilaas T, van der Horst IC, et al. Cardiac death and reinfarction after 1 year in the Thrombus Aspiration during Percutaneous coronary intervention in Acute myocardial infarction Study (TAPAS): a 1-year follow-up study. Lancet. 2008 Jun 7;371(9628):1915-20. [3] Lefevre T and Louvard Y. Description and management of difficult anatomy encountered during transradial intervention. In: M. Hamon and E. McFadden, Editors, Transradial approach for cardiovascular interventions, Europa Stethoscope Media, Carpiquet (2003),241-254.

[4] Rao SV, Ou FS, Wang TY, et al. Trends in the prevalence and outcomes of radial and femoral approaches to percutaneous coronary intervention: a report from the National Cardiovascular Data Registry. JACC Cardiovasc Interv. 2008 Aug;1(4):379-86.

Corresponding author information: Name: Roman Surname: Romero-Ortuno Email: romeror@tcd.ie Affiliation: Department of Medicine for the Elderly, St James's Hospital, James's Street, Dublin 8, Ireland

Frailty: the great confounder, the great forgotten

To the editor: Ryan, Steen, Seifer, et al. [1] present the results of SAFE PACE-2, which are at odds with SAFE PACE-1 [2]. The authors discuss that this may be due to greater frailty in SAFE PACE-2 participants. This point is valid and merits further reflection in relation to recent frailty literature.

Frailty is a well recognised clinical syndrome, but remains difficult to define and measure. Central to the concept of frailty is the dysregulation of multiple systems (e.g. balance, muscle strength, cognition), all of which independently contribute to the high incidence of falls in frail older people [3].

If falls can be a hallmark of frailty, any research on interventions with falls as endpoint should be able to control for this confounder. Many frailty assessment tools have been (and are still being) proposed, but are rarely used to help interpret results of trials in geriatric medicine (e.g. by using frailty scales as covariates, or conducting subgroup analyses based on increasing frailty categories).

The above would help establish which types of patients are most likely to benefit from an intervention. Along these lines, Ryan, Steen, Seifer, et al. [1] argue that the main beneficiaries of pacing may be non-frail patients, who are at low risk of falls from other sources. It is reasonable to presume that frail patients will continue to fall, despite minimising the contributing effect of carotid sinus hypersensitivity.

The issue calls for a frailty-adjusted meta-analysis of all trials of pacing for carotid sinus hypersensitivity, before the intervention is regarded as lacking evidence. The point by Alboni, Dinelli, Gianfranchi L, et al. [4] remains valid, in that the treatment for recurrent vasovagal syncope âÃÆ’¢Ã‚‚¬ÃÆ’‹Ã‚Ã…“can be chosen by considering the clinical context, the risk of trauma and possible comorbidities, in addition to utilizing the little or controversial knowledge available, as well as common sense'.

Older people are very heterogeneous. We need frailty measures that serve as common language for comparing studies that, whilst asking the same questions and employing the same methodology, happened to recruit from different populations. This would contribute towards a better evidence base in Geriatric Medicine.

References:

1 Ryan D, Steen N, Seifer C, et al. Carotid Sinus Syndrome and falls, should we pace? A multi-centre, randomised control trial (Safepace 2). Heart 2009. 2 Kenny RA, Richardson DA, Steen N, et al. Carotid sinus syndrome: a modifiable risk factor for nonaccidental falls in older adults (SAFE PACE). J Am Coll Cardiol 2001;38:1491-6. 3 Nowak A, Hubbard RE. Falls and frailty: lessons from complex systems. J R Soc Med 2009;102:98-102. 4 Alboni P, Dinelli M, Gianfranchi L, et al. Current treatment of recurrent vasovagal syncope: between evidence-based therapy and common sense. J Cardiovasc Med (Hagerstown) 2007;8:835-9.

To the Editor: Ryan et al. report on the efficacy of Dual Chamber pacemaker implantation in patients with cardio-inhibitory carotid sinus hypersensitivity (CICSH) and falls in SAFEPACE-2 (Syncope And Falls in the Elderly- Pacing And Carotid sinus Evaluation)[1]. This study had the potential to expand on the findings of SAFEPACE-1 [2] and address some of the weaknesses of the latter with a blinded, multicenter, and less select cohort [3]. However, despite improved external validity, SAFEPACE-2 reports findings at odds with the prior results of SAFEPACE-1 by demonstrating that the null hypothesis was correct (pacemaker implantation did not reduce falls in CICSH)[1].

The authors of SAFEPACE-2 are to be applauded for their efforts to increase the generalizability of their results and for their attention to detail with regards to data acquisition and analysis. This begs the question, why the marked difference in findings between the two SAFEPACE trials [1-2]? While it is true that the cohort in SAFEPACE-2 had more comorbidity, one wonders whether further review of the trial methodology will yield another explanation.

The ‘double-blind’ design of SAFEPACE-2 seems difficult to achieve given the nature of the intervention. Pacemaker insertion requires the patient to carry a specific pacemaker card and to follow-up at specialized pacemaker clinics. In contrast, a loop recorder requires specific education as the patient self-activates the recorder with a hand-held device. Failure to blind the patients could significantly affect the primary outcome of self-reported falls, increasing the potential for recall bias in favor of the intervention. Therefore, this methodological issue may actually strengthen the author’s findings in SAFEPACE 2 and does not explain the difference in results between the trials.

At first glance, the difference may be explained by the lack of statistical power in SAFEPACE-2. It is true that SAFEPACE 2 is underpowered to detect a difference of 20% in the number of patients who fell, however it is almost fully powered to detect a difference of 40%. This was the power criteria used in SAFEPACE 1 [2]. Therefore, lack of statistical power also does not fully explain the difference in results between the trials.

One methodological issue which may account for the different trial results is the ‘randomization to implantation’ time. The overall relative risk (RR) for falls with pacemaker implantation in SAFEPACE-2 was 0.79 (95% Confidence Interval [CI], 0.4-1.5), but was 0.23 (95% CI, 0.15-0.32) when comparing patients before and after device implantation [1]. The latter RR suggests that device implantation made a difference to fall rates and raises the possibility that the overall result was obscured by a prolonged ‘randomization to implantation’ time. Given the multicenter nature of this trial it seems likely that this time was longer in SAFEPACE -2 than the single centre SAFEPACE-1. Therefore, it seems possible that inclusion of fall data prior to device implantation (the intervention) obscured the result of SAFEPACE-2 and may partially explain the difference in results between the two SAFEPACE trials.

Reporting the mean and median time from ‘randomization to implantation’, and exclusion of the pre-implantation fall data from the analysis may help shed more light on this important issue.

John W. McEvoy M.B., M.R.C.P.I. The Johns Hopkins Hospital 600 N. Wolfe Street Baltimore, Maryland 21287 Jmcevoy1@jhmi.edu

1. Ryan D, Steen N, Seifer C, Kenny RA. Carotid Sinus Syndrome and falls, should we pace? A multi-centre, randomised control trial (Safepace 2). Heart 2009. 2. Kenny RA, Richardson DA, Steen N, Bexton RS, Shaw FE, Bond J. Carotid sinus syndrome: a modifiable risk factor for nonaccidental falls in older adults (SAFE PACE). J Am Coll Cardiol 2001;38(5):1491-6. 3. McAnulty JH. Carotid sinus massage in patients who fall: will it define the role of pacing? J Am Coll Cardiol 2001;38(5):1497.

November 11, 2009 Editor, Heart British Medical Journal Dear Sir: I am writing to comment on the excellent article by Bhaskaran et al in Heart[1], and especially on the editorial by David Newby [2] that commented on this paper. In my opinion, Dr. Newby has missed the most important conclusion of the Bhaskaran paper. Dr. Newby’s editorial was focused mainly on the cardiac effects of fine particulate pollution, and included a graph of data from Beijing, China. However, it seems to me that a far more important contribution of the Bhaskaran paper was the observation of an “ozone protective effect” in several parts of the world. The authors pointed out that this effect is probably due to some pollutant that is negatively correlated with ozone, and cites my previous paper[3] suggesting that the effect could be due to unsuspected methyl nitrite (MN) in the air. This hypothesis has a high degree of plausibility because it is known that MN, unlike ozone, is rapidly destroyed by sunlight and so would be negatively correlated with ozone. To the best of my knowledge, this ozone protective effect is totally inexplicable unless an unknown pollutant, such as MN, is present. If Dr. Newby’s point of view is to be accepted, then presumably he must argue that fine particulate pollution is also the cause of the ozone protective effect. However, that hypothesis has been thoroughly discredited in another paper [4]. In that paper I showed that fine particulate matter can not explain the negative ozone associations in any parts of the world in which there is published evidence for the negative effects. I particularly showed that explanation is extremely unlikely in Hong Kong, China. Hence, I feel that the most important contribution of the Bhaskaran paper is to alert the world to the possible existence of a very important toxic pollutant whose presence has escaped attention. Most desperately needed is funding for research to identify MN in engine exhaust. To date, such funding has not been available in the United States. Sincerely, Professor Peter M. Joseph, Ph.D. School of Medicine University of Pennsylvania Philadelphia, PA, USA email = joseph@rad.upenn.edu REFERENCES 1. Bhaskaran K, Hajat S, Haines A, Herrett E, Wilkinson P, Smeeth L. Effects of air pollution on the incidence of myocardial infarction. Heart 2009;95:1746-1759. 2. Langrish JP, Mills NL, Newby DE. Heat and haze: a forecast for myocardial infarction? Heart 2009;95:1721-1722. 3. Joseph PM. Paradoxical ozone associations could be due to methyl nitrite from combustion of methyl ethers or esters in engine fuels. Environ Int 2007;33:1090-106. 4. Joseph PM. Can fine particulate matter explain the paradoxical ozone associations? Environ Int 2008;34:1185-91.