Abstract
Introduction
Electrocardiogram (ECG) monitoring is an important tool to detect and mitigate the risk of potentially fatal drug-induced QT prolongation and remains fundamental in supporting the quality use of high-risk QT interval prolonging medicines.
Objective
The aim of this systematic review was to determine the prevalence of baseline and/or follow-up ECG use in adult patients taking high-risk QT interval prolonging medicines in clinical practice.
Methods
CINAHL, Cochrane Library, Embase, PubMed, EThOS, OpenGrey and Proquest were searched for studies in adults that reported ECG use at baseline and/or at follow-up in relation to the initiation of a high-risk QT interval prolonging medicine in any clinical setting; either hospital or non-hospital. Two reviewers independently assessed the methodological quality of included studies. Proportional meta-analysis was conducted with all studies reporting baseline ECG use, before medicine initiation, and follow-up ECG use, within 30 days of medicine initiation.
Results
There was variability in baseline ECG use according to the practice setting. The prevalence of baseline ECG use for high-risk QT interval prolonging medicines was moderate to high in the hospital setting at 75.1% (95% CI 64.3–84.5); however, the prevalence of baseline ECG use was low in the non-hospital setting at 33.7% (95% CI 25.8–42.2). The prevalence of follow-up ECG use was low to moderate in the hospital setting at 39.2% (95% CI 28.2–50.8) and could not be determined for the non-hospital setting.
Conclusions
The use of ECG monitoring for high-risk QT interval prolonging medicines is strongly influenced by the clinical practice setting. Baseline ECG use occurs more in the hospital setting in comparison to the non-hospital setting. There is lower use of follow-up ECG in comparison to baseline ECG.
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High-risk QT interval prolonging medicines have compelling evidence for risk of torsades de pointes (TdP) and ECG monitoring remains unequivocally recommended for their use. |
The use of ECG for drug safety monitoring of high-risk QT interval prolonging medicines in clinical practice is variable and limited. |
There is a clear lack of policy and research for ECG monitoring of high-risk QT interval prolonging medicines in the non-hospital setting. |
1 Introduction
Medicines with the potential to cause QT prolongation belong to a wide spectrum of therapeutic classes and their use is expected in all types of healthcare settings. It has previously been estimated that the use of QT interval prolonging medicines could result in > 15,000 deaths annually in the US and Europe [1]. Therefore, prevention of this adverse drug reaction remains a fundamental consideration of therapeutic decision making in all areas of clinical practice.
QT prolongation remains the best measure, although an imperfect predictor [2, 3], for the more serious risk of torsades de pointes (TdP) and sudden cardiac death (SCD). Electrocardiographic (ECG) monitoring remains the best available tool to assess and mitigate the risk of TdP [4, 5], and hence support the safe use of high-risk QT interval prolonging medicine therapy.
Since 2004, guidelines published by the American Heart Association (AHA) have recommended the use of ECG monitoring before and after the commencement of high-risk QT interval prolonging medicines [6,7,8]. These guidelines have generally focussed on medicines used in the hospital setting. In contrast to the hospital setting, there is very limited guidance for ECG monitoring specifically relating to prevention of drug-induced QT prolongation in non-hospital settings. Trinkley et al. (2013) [5] recommended that risk mitigation strategies and QT interval monitoring are needed in every care setting. Despite this notion, very few recommendations have been published specifically relating to the non-hospital setting [9, 10].
There has been a strong emphasis on ECG monitoring of hospitalised patients as they are considered at greater risk of QT prolongation and TdP due to the increased prevalence of risk factors. However, complex patients with multiple risk factors for QT prolongation and TdP are increasingly being managed in non-hospital settings such as outpatient clinics, primary care and in residential care facilities. Although differing healthcare systems, personnel and equipment influence the feasibility of risk management strategies, medicines safety and patient management principles in relation to high-risk QT interval prolonging medicines remain the same.
Initiation of high-risk QT interval prolonging medicines, and indeed non–high-risk QT interval prolonging medicines, in contrast to their continuing use, has compelling cause for ECG monitoring and provides a clear platform on which to summarise the prevalence of ECG use, in all areas of clinical practice, at key points of therapeutic decision making. The objective of this review was to determine the prevalence of ECG monitoring conducted at baseline and the prevalence of ECG monitoring conducted at follow-up, for patients taking high-risk QT interval prolonging medicines, in any clinical setting.
2 Methods
The JBI (formerly Joanna Briggs Institute) methodological approach to systematic reviews of prevalence and incidence was followed [11, 12]. Reporting of this review is in accordance with the Preferred Reporting Items for Systematic Reviews and Meta-Analysis (PRISMA) guidelines [13]. The study protocol was previously published [14] and registered with the International Prospective Register of Systematic Reviews (PROSPERO, CRD42021240762).
2.1 Inclusion and Exclusion Criteria
Inclusion was restricted to adults (aged ≥ 18 years) initiated on a high-risk QT interval prolonging medicine, rather than on stable or ongoing medicine therapy. Medicines listed in the ‘known risk of TdP’ category, as defined by the University of Arizona Center for Education and Research on Therapeutics (AZCERT) [15], were considered high-risk medicines for this systematic review. Medicines that were not classified as 'known risk of TdP' at the time of original study were excluded from the review.
Baseline ECG was included if conducted at any time prior to the initiation of a high-risk QT interval prolonging medicine. Follow-up ECG had to occur within 30 days from medicine initiation. Follow-up ECG that occurred due to a raised QT threshold at baseline ECG were excluded.
ECG use was excluded if described in any way other than a discrete non-continuous ECG test. Studies intentionally conducting ECGs were excluded.
Any study types, except for case studies and case series, were considered, from any country and conducted in any clinical setting including any hospital and non-hospital settings.
2.2 Search Strategy and Study Selection
A comprehensive search was conducted on 15 February 2021. Published studies were searched using CINAHL (EBSCO), Cochrane Library, Embase (Ovid) and MEDLINE (PubMed). Conference abstracts were excluded. Unpublished studies were searched using EThOS, OpenGrey and ProQuest Dissertations and Theses Global. No language restrictions were applied. See Electronic Supplementary Material (ESM) 1 for the full search strategy.
The search start date was 2004, relating to the first prominent practice standards discussing ECG monitoring of high-risk QT interval prolonging medicines [6].
All titles and abstracts identified by the searches were screened for inclusion using Endnote X9 (Clarivate Analytics, PA, USA), and potentially relevant articles were retrieved in full. Duplicates were initially identified automatically in Endnote X9 and then manually following automation. To assist study selection, authors of papers were contacted to request additional data for clarification.
Any uncertainties were resolved through discussion with a second reviewer (MW). The reference lists of all studies selected for quality assessment were screened for additional studies.
2.3 Quality Assessment
Quality assessment of eligible studies was undertaken independently by two reviewers (MP, CB) using a standardised critical appraisal instrument from JBI for studies reporting prevalence data [11, 12, 16].
Any discrepancies were resolved through discussion between the two reviewers (MP, CB) or with a third reviewer (MW). Authors of papers were contacted to request missing or additional data for clarification.
The assessment criteria of the critical appraisal instrument were adapted to suit the needs of this review. Specifically, domain four of the instrument involved whether the clinical setting was sufficiently described to be able to identify its place in the healthcare system. Domain seven involved whether the time frames for baseline and/or follow-up ECG were described clearly.
To be eligible to be deemed of high-quality, studies had to perform well on domains four and seven and had to achieve a total score of at least seven out of nine on the critical appraisal instrument.
2.4 Data Extraction
Data was extracted using a modified version of the JBI standardised data extraction instrument [11], including population characteristics, high-risk medicines studied, information about baseline and/or follow-up ECG use, reasons for ECG, and details of the clinical setting. Any ambiguities associated with data extraction were resolved following discussion with a second reviewer (MW).
Sample size related to the total cohort of patients on newly initiated high-risk QT prolonging medicine(s) only. Studies with pre-intervention and post-intervention cohorts were extracted as two separate samples, which are identified in this review as data group (a) and data group (b), respectively.
ECG use data that were reported separately for different cohorts based on various descriptors such as specific clinical locations were combined into a single sample.
2.5 Data Synthesis
Studies were pooled with proportional meta-analysis using the JBI System for Unified Management, Assessment and Review of Information (JBI SUMARI) [17].
Results of each individual study included numerator and denominator for ECG use at baseline and for ECG use at follow-up, proportion (expressed as a percentage) and 95% confidence intervals (CIs). The Freeman-Tukey transformation was used for the meta-analysis. Proportions were pooled using the random effects model due to the heterogeneity between studies [18] and reported as a percentage with a 95% CI. Forest plots were used to display the results. Heterogeneity was reported using the I2 statistic. Publication bias was not assessed, as there is no evidence that proportional data adequately adjusts for these tests [18].
Separate analyses were conducted for each category of baseline ECG use and follow-up ECG use and additionally within these groups, according to clinical setting (hospital setting and non-hospital setting). Furthermore, sensitivity analyses were conducted to determine the impact of exclusion of poor-quality studies; ‘leave one (or more) out’ analyses were conducted where there were sufficient study level reasons to explore the impact of exclusion of individual studies with biases not otherwise accounted for by quality assessment. All analyses were conducted with at least two studies in each category.
3 Results
Searches of databases returned 9871 records. Following the removal of duplicates, the titles and abstracts of 6548 unique records were screened. Following the exclusion of 6460 records, 88 were eligible for full-text review. Three non-English records (all French) were identified, two of which could not be located and one of which had an English abstract which was used to determine eligibility. Multiple reports of the same study were not identified. Seventy-four studies were excluded. See ESM 2 for reasons for exclusion of full-text studies. Fourteen studies (14 reports) were included, all of which were retrospective cohort studies (Fig. 1).
Flow diagram of search results and review process (PRISMA 2020) [13]
Thirteen studies included data relating to baseline ECG use, involving 18,581 participants. Only seven studies included data relating to follow-up ECG use, involving 43,321 participants.
3.1 Study Characteristics
Characteristics of the included studies are reported in Table 1. Most studies were conducted in the hospital setting. Hospital settings were heterogenous, including an emergency department, various clinical units including general medicine, cardiology and psychiatry and there was one inpatient headache centre. Many studies did not describe the specific location of hospital care, rather describing patients in other ways such as “total hospital population” [19], “medically ill and/or hospitalised inpatients” [20, 21], “inpatients” [22, 23] and “admitted patients” [24].
Three studies involved pre-intervention and post-intervention cohorts, which are identified in this review as data group (a) and data group (b), respectively. The intervention in two studies, Forbes et al. [23] and Dunker et al. [24], was passive in nature, in which ECG use was determined relative to the publication of a national public health warning relating to drug-induced QT prolongation. The intervention in the study by Muzyk et al. [20] was active in nature, in which ECG use was determined relative to the implementation of a computerised physician order entry set which involved generation of automated baseline and daily ECG orders in all patients prescribed the medicine of interest. The pre-intervention and post-intervention cohorts in each study involved two separate data sets (Table 1).
3.2 Methodological Quality
Methodological quality was deemed to be high for five out of 14 studies. See ESM 3 for assessment of methodological quality.
Two studies involved very large cohorts in the thousands and all other studies involved small to very small cohorts of < 100 or in the low hundreds.
Three studies involved additional biases that were not recognised in the formal assessment of methodological quality. Cole et al. [25] involved a medicine which was only deemed high-risk for 1 out of 5 years of their study period (R. Woosley, personal communication, 19 October 2021). Robbins et al. [26] specified that baseline ECG was obtained in all patients, and it is not clear within the study whether baseline ECG was conducted intentionally. Muzyk et al. [20] (b) involved active intervention of ECG monitoring behaviour through automated baseline and daily ECG orders following prescription of high-risk medicine.
3.3 Prevalence of Baseline ECG Monitoring
The prevalence of baseline ECG monitoring for high-risk QT interval prolonging medicines was strongly influenced by the practice setting.
The prevalence of baseline ECG monitoring in the hospital setting (11 studies, n = 18,264) was generally moderate to high with a pooled proportion estimate of 73.0% (95% CI 57.0–86.5). Removing studies identified with additional biases from the analysis due to their previously described limitations, the prevalence estimate in the consequent analysis (9 studies, n = 1577) was only marginally increased to 75.1% (95% CI 64.3–84.5) (Fig. 2).
Proportional meta-analysis of baseline ECG use—hospital setting only and leave three out (studies with additional biases)
By removing the poor-quality studies from the analysis of the hospital setting, the final pooled proportion in the consequent analysis (4 studies, n = 17,188) was moderately reduced to 58.6% (95% CI 21.9–90.5).
However, by removing poor-quality studies and studies identified with additional biases from the analysis, the final pooled proportion in the consequent analysis (3 studies, n = 642) was corrected upward to 74.3% (95% CI 48.9–93.2).
Heterogeneity for all these baseline ECG pooled proportion estimates was considerable and demonstrated by I2 > 90%.
In contrast with studies conducted in the hospital setting, the prevalence of baseline ECG monitoring in the non-hospital settings were much lower. The pooled proportion estimate for the non-hospital setting (2 studies, n = 317), was calculated to be 33.7% (95% CI 25.8–42.2) (Fig. 3). Heterogeneity was only moderate in this analysis, described by an I2 value of 60, however this was not statistically significant (p = 0.1138).
Proportional meta-analysis of baseline ECG use—non-hospital setting only
3.4 Prevalence of Follow-up ECG Monitoring
In comparison with baseline ECG monitoring, uptake of follow-up ECG monitoring was generally poorer. The prevalence of follow-up ECG monitoring in the non-hospital setting could not be determined due to lack of studies.
The prevalence of follow-up ECG monitoring in the hospital setting was low to moderate. The pooled proportion estimate in the hospital setting (6 studies, n = 17,091) was 34.2% (95% CI 22.7–46.7). By removing studies with additional biases from the analysis of the hospital setting, due to their previously described limitations, the pooled proportion in the consequent analysis (5 studies, n = 461) was marginally increased to 39.2% (95% CI 28.2–50.8) (Fig. 4). The heterogeneity of these pooled proportion estimates was considerable, described by I2 values of 94.9% and 81.6%, respectively.
Proportional meta-analysis of follow-up ECG use—hospital setting only and leave two out (studies with additional biases)
Removing poor-quality studies from the analysis of the hospital setting considerably reduced the prevalence estimate, and the pooled proportion in the consequent analysis (2 studies, n = 16,768) was 21.9% (95% CI 4.7–46.9) (Fig. 5). However, one the two remaining studies in this analysis involved additional bias not recognised in the formal assessment of methodological quality. Heterogeneity was considerable in this analysis, described by I2 = 98.5%.
Proportional meta-analysis of follow-up ECG use—hospital setting only and high-quality studies only; any clinical setting and high-quality studies only
The prevalence of follow-up ECG monitoring in any clinical practice setting (7 studies, n = 43,321) included only one additional study, in comparison to the prevalence of follow-up ECG monitoring in the hospital setting. The additional study did not specify the healthcare setting in which medicine prescription or ECG use occurred and included the largest cohort out of all the studies in the review, involving more than 20,000 patients. The prevalence of follow-up ECG monitoring in any clinical setting was lower in comparison to the prevalence of follow-up ECG monitoring in the hospital setting, and the pooled proportion estimate was calculated to be 33.6% (95% CI 23.7–44.3). Heterogeneity was considerable, described by I2 = 99.6%. By removing studies with additional biases from the analysis of any clinical practice setting, the pooled proportion of the consequent analysis (6 studies, n = 26,708) was only slightly reduced to 32.7% (95% CI 29.1–36.5) (Fig. 6). Heterogeneity was only moderate, described by an I2 of 38.3, although was not statistically significant (p = 0.1675).
Proportional meta-analysis of follow-up ECG use—any clinical setting and leave two out (studies with additional biases)
Removing the poor-quality studies from the analysis of any clinical practice setting, the pooled proportion of the consequent analysis (2 studies, n = 16,768) was 21.9% (95% CI 4.7–46.9) (Fig. 5) and in fact provided the same result as for the prevalence of follow-up ECG monitoring in the hospital setting with poor-quality studies removed.
The Grading of Recommendations, Assessment, Development and Evaluations (GRADE) approach, based on the assessment of evidence about prognosis [33], was utilised to generate a Summary of Findings (Table 2).
4 Discussion
The focus of this review was to determine the prevalence of ECG monitoring in relation to high-risk QT interval prolonging medicines, to aid in the understanding of the likely utilisation of this risk management strategy in real-world clinical practice settings.
Low or inadequate use of ECG monitoring in relation to the prevention of drug-induced QT prolongation has been widely acknowledged and reported [4, 10, 32, 34,35,36,37,38]. This is the first systematic review to summarise the prevalence of ECG use for high-risk QT interval prolonging medicines in clinical practice.
This review indicates that the prevalence of ECG monitoring seems to be influenced by the clinical practice setting, in which baseline ECG monitoring occurs with reasonable frequency in the hospital setting, and much less commonly in the non-hospital setting. Follow-up ECG monitoring, specifically in the hospital setting, occurs far less frequently than baseline ECG monitoring. Overall, there is sparse evidence that any type of ECG monitoring occurs in the non-hospital setting. On the basis of the studies identified in this review there is a need to improve the strength of evidence of the reported prevalence estimates relating to both baseline and follow-up ECG monitoring. There is a need for larger studies, in a greater variety of clinical settings, across a wider variety of countries. Furthermore, well conducted studies are needed, including with clear reporting and distinction of included medicines, clearly articulated timeframes for ECG monitoring in relation to medicine therapy, and clear reporting of reasons for ECG use.
There was very limited reporting on the reason for ECG monitoring, and it is unknown if the use of ECG monitoring was related in any way to specifically monitoring the QT interval. Only one study in the entire review reported the reasons for use of ECG, and only 4.7% of ECG use was determined to relate to QT monitoring [26]. Hence, it is possible that the use of ECG monitoring for high-risk QT interval prolonging drugs is overestimated, and therefore the prevalence estimates for both baseline and follow-up ECG monitoring are lower than reported. Certainly, ECG use is undertaken more readily in hospitalised patients in the context of investigation of acute illness. The moderate to high prevalence estimates of baseline ECG monitoring of high-risk QT interval prolonging medicines could possibly be an artefact of hospitalisation rather than QT monitoring for the purposes of drug safety management per se. Hospitalisation itself may provide a high probability of safeguard for ECG monitoring for those commenced on a high-risk QT interval prolonging medicine; however, this is probably less likely for those that are not hospitalised.
Other reasons can contribute to the limited use of ECG monitoring for high-risk QT interval prolonging medicines. It has been recognised that clinicians are often unable to identify the medicines and risk factors that can prolong the QT interval [39]. Furthermore, it has been recognised that clinicians have difficulty in accurately measuring a QT interval, and clinicians frequently ignore QT prolongation even if it is recognised [40].
Mortality and morbidity outcomes and economic impact associated with use of ECG in relation to drug-induced QT prolongation still remain unknown [10, 41, 42], largely due to the low absolute risk of TdP and SCD [34]. Despite lack of evidence for these important endpoints, ordering an ECG before and during therapy with high-risk QT interval prolonging medicines remains a practical and reliable risk management strategy to support the safe use of QT interval prolonging medicine therapy.
This review gives prominence to the lack of policy and research for use of ECG monitoring in non-hospital settings. The prescribing of QT interval prolonging medicines is reported to have at least doubled in recent times [37]. Several studies report that prescription of QT prolonging medicines is common in outpatient settings [43, 44]. It is well recognised that the use of QT prolonging medicines in other non-hospital settings such as community-based primary care practice and residential care facilities is also common [45].
Policies and guidelines alone are likely not enough to ensure use of ECG monitoring in practice, as highlighted by this review. Practical approaches are needed to improve use of ECG monitoring and risk mitigation of drug-induced QT prolongation.
There is still great potential for digital technologies to be leveraged to improve the management of drug-induced QT prolongation. Simpler and more accessible methods to monitor QT, such as wearable digital devices, may offer a solution for the non-hospital settings. However, these remain immature and unvalidated in the context of drug-induced QT prolongation and further research is needed to confirm the feasibility of these [39, 46, 47]. Further development of remote monitoring for drug safety management is likely to be supported by improving awareness of drug safety benefits of both clinicians and consumers.
Although clinical decision support tools relating to QT interval prolonging medicines have been developed, these have been associated with limitations [46, 48,49,50]. Alternative information management systems such as data-driven drug-induced QT prolongation surveillance using adverse reaction signals derived from electrocardiogram data [51] are only just emerging and may hold important solutions to improve drug safety management at the point of care. Access to, and clinicians’ awareness of, reliable online information sources of QT interval prolonging medicines are not well reported yet may be a simple and effective strategy to improve identification and risk management of the highest risk QT interval prolonging medicines.
4.1 Limitations
Most studies in this review involved small samples, and studies often occurred in very specialised practice settings, mostly represented by hospital settings where there is likely reliable access to ECG monitoring. There was very limited representation of non-hospital, in particular, non-inpatient settings; there was no representation of community-based primary care practice.
This review focussed on comparison of ECG use in the hospital and non-hospital settings and did not investigate ECG use according to specific clinical areas or units. Furthermore, the review did not include use of continuous ECG monitoring. Both types of information would be important in strengthening understanding of ECG use trends.
There are numerous facets of complexity in the use of ECG monitoring in relation to drug safety and management of QT interval prolonging medicines. These include the feasibility of ECG use, clinicians’ skill and expertise in relation to ECG use and more specifically, QT interval monitoring, clinicians’ awareness of QT interval prolonging potential of medicines and understanding clinicians’ actual therapeutic decision-making process. Prevalence estimates by themselves do not provide insights into any of these elements. Qualitative research would be beneficial to fully explore the complex clinical decision-making process of high-risk QT interval prolonging medicine use, and also the use of risk management strategies including ECG monitoring. Improved quantitative evidence complemented by qualitative data provides the ultimate basis on which to determine the most effective improvement strategies in relation to drug safety and management of QT interval prolonging medicines.
5 Conclusions
Use of ECG monitoring is a key strategy to reduce risk of the potentially fatal adverse reaction that is drug-induced QT prolongation. This review highlights the limited and variable use of both baseline and follow-up ECG monitoring of high-risk QT interval prolonging medicines in adult patients in clinical practice. There is a clear lack of information on the use of ECG monitoring in non-inpatient and non-hospital settings. This review also highlights the need for research in these under-recognised healthcare settings to aid safe use of high-risk QT interval prolonging medicines.
Change history
20 October 2022
Missing Open Access funding information has been added in the Funding Note.
References
Straus SM, et al. Non-cardiac QTc-prolonging drugs and the risk of sudden cardiac death. Eur Heart J. 2005;26(19):2007–12.
Schwartz PJ, Woosley RL. Predicting the unpredictable: drug-induced QT prolongation and torsades de pointes. J Am Coll Cardiol. 2016;67(13):1639–50.
QT interval and drug therapy. BMJ. 2016;353:i2732.
Jardin CG, Putney D, Michaud S. Assessment of drug-induced torsade de pointes risk for hospitalized high-risk patients receiving QT-prolonging agents. Ann Pharmacother. 2014;48(2):196–202.
Trinkley KE, et al. QT interval prolongation and the risk of torsades de pointes: essentials for clinicians. Curr Med Res Opin. 2013;29(12):1719–26.
Drew BJ, et al. Practice standards for electrocardiographic monitoring in hospital settings: an American Heart Association scientific statement from the Councils on Cardiovascular Nursing, Clinical Cardiology, and Cardiovascular Disease in the Young: endorsed by the International Society of Computerized Electrocardiology and the American Association of Critical-Care Nurses. Circulation. 2004;110(17):2721–46.
Drew BJ, et al. Prevention of torsade de pointes in hospital settings: a scientific statement from the American Heart Association and the American College of Cardiology Foundation. J Am Coll Cardiol. 2010;55(9):934–47.
Tisdale JE, et al. Drug-induced arrhythmias: a scientific statement from the American Heart Association. Circulation. 2020;142:e214–33.
de Lemos ML, et al. Approach to initiating QT-prolonging oncology drugs in the ambulatory setting. J Oncol Pharm Pract. 2019;25(1):198–204.
Xiong GL, et al. QTc monitoring in adults with medical and psychiatric comorbidities: expert consensus from the Association of Medicine and Psychiatry. J Psychosom Res. 2020;135: 110138.
Munn Z, Moola S, Lisy K, Riitano D, Tufanaru C. Systematic reviews of prevalence and incidence, Chapter 5. In: Aromataris E, Munn Z, editors. Joanna Briggs Institute Reviewer's Manual. The Joanna Briggs Institute; 2017. https://reviewersmanual.joannabriggs.org/.
Munn Z, Moola S, Lisy K, Riitano D, Tufanaru C. Methodological guidance for systematic reviews of observational epidemiological studies reporting prevalence and incidence data. Int J Evid Based Healthc. 2015;13:147–53.
Page MJ, et al. The PRISMA 2020 statement: an updated guideline for reporting systematic reviews. BMJ. 2021;372: n71.
Putnikovic M, Ward M, Jordan Z. Use of ECG monitoring for adult patients taking high-risk QT interval-prolonging drugs in clinical practice: a systematic review protocol. JBI Evid Synth. 2021;19(11):3113–20.
Woosley R, Heise CW, Romero KA. http://www.crediblemeds.org [cited 11 April 2020].
Munn Z, et al. The development of a critical appraisal tool for use in systematic reviews addressing questions of prevalence. Int J Health Policy Manag. 2014;3(3):123–8.
Munn Z, Aromataris E, Tufanaru C, Stern C, Porritt K, Farrow J, Lockwood C, Stephenson M, Moola S, Lizarondo L, McArthur A. The development of software to support multiple systematic review types: the Joanna Briggs Institute System for the Unified Management, Assessment and Review of Information (JBI SUMARI). Int J Evid Based Healthc. 2019;17:36–43.
Barker TH, et al. Conducting proportional meta-analysis in different types of systematic reviews: a guide for synthesisers of evidence. BMC Med Res Methodol. 2021;21(1):189.
Vandael E, et al. Risk management of QTc-prolongation in patients receiving haloperidol: an epidemiological study in a University hospital in Belgium. Int J Clin Pharm. 2016;38(2):310–20.
Muzyk AJ, et al. A computerized physician order entry set designed to improve safety of intravenous haloperidol utilization: a retrospective study in agitated hospitalized patients. Drug Saf. 2012;35(9):725–31.
Atayee RS, et al. Methadone inpatient and discharge prescribing patterns for pain at an academic health system. J Palliat Med. 2017;20(2):184–92.
Cheung D, et al. Unsafe use of intravenous haloperidol: evaluation of recommendation-concordant care in hospitalized elderly adults. J Am Geriatr Soc. 2013;61(1):160–1.
Forbes N, et al. Domperidone prescribing practices exposed patients to cardiac risk despite a “black box” warning: a Canadian tertiary care center study. Can J Gastroenterol Hepatol. 2016;2016:2937678.
Dunker A, et al. Impact of the FDA warning for azithromycin and risk for QT prolongation on utilization at an academic medical center. Hosp Pharm. 2016;51(10):830–3.
Cole JB, et al. The incidence of QT prolongation and torsades des pointes in patients receiving droperidol in an urban emergency department. West J Emerg Med. 2020;21(4):728–36.
Robbins NM, et al. Safety of domperidone in treating nausea associated with dihydroergotamine infusion and headache. Neurology. 2016;87(24):2522–6.
Girgis SJ, Maroney ME, Liu MT. Evaluation of the use of electrocardiogram monitoring in patients on psychotropic medications that have a risk of QT prolongation. Ment Health Clin. 2016;6(4):171–7.
Choo WK, et al. Prescribers’ practice of assessing arrhythmia risk with QT-prolonging medications. Cardiovasc Ther. 2014;32(5):209–13.
Macey TA, et al. Patterns of care and side effects for patients prescribed methadone for treatment of chronic pain. J Opioid Manag. 2013;9(5):325–33.
Manchia M, et al. Clinicians’ adherence to clinical practice guidelines for cardiac function monitoring during antipsychotic treatment: a retrospective report on 434 patients with severe mental illness. BMC Psychiatry. 2017;17(1):121.
Ehrenpreis ED, et al. Domperidone is commonly prescribed with QT-interacting drugs: review of a community-based practice and a postmarketing adverse drug event reporting database. J Clin Gastroenterol. 2017;51(1):56–62.
Pezo RC, et al. Underuse of ECG monitoring in oncology patients receiving QT-interval prolonging drugs. Heart. 2019;105(21):1649–55.
Iorio A, et al. Use of GRADE for assessment of evidence about prognosis: rating confidence in estimates of event rates in broad categories of patients. BMJ. 2015;350: h870.
Warnier MJ, et al. Are ECG monitoring recommendations before prescription of QT-prolonging drugs applied in daily practice? The example of haloperidol. Pharmacoepidemiol Drug Saf. 2015;24(7):701–8.
Berling I, et al. A review of ECG and QT interval measurement use in a public psychiatric inpatient setting. Australas Psychiatry. 2018;26(1):50–5.
Ali Z, et al. Prevalence of QTc interval prolongation and its associated risk factors among psychiatric patients: a prospective observational study. BMC Psychiatry. 2020;20(1):277.
Schachtele S, et al. Co-prescription of QT-interval prolonging drugs: an analysis in a large cohort of geriatric patients. PLoS One. 2016;11(5): e0155649.
Mareedu RK, et al. Abstract 1200: QT-prolonging medication prescription tendencies in a cohort of hospitalized patients with known long QT intervals. Circulation. 2008;118(suppl 18):S1084.
Zolezzi M, Cheung L. A literature-based algorithm for the assessment, management, and monitoring of drug-induced QTc prolongation in the psychiatric population. Neuropsychiatr Dis Treat. 2018;15:105–14.
Gibbs C, et al. Predictors of mortality in high-risk patients with QT prolongation in a community hospital. Europace. 2018;20(Fi1):f99–107.
Simoons M, et al. Limited evidence for risk factors for proarrhythmia and sudden cardiac death in patients using antidepressants: Dutch consensus on ECG monitoring. Drug Saf. 2018;41(7):655–64.
Al-Khatib SM, et al. What clinicians should know about the QT interval. JAMA. 2003;289(16):2120–7.
Curtis LH, et al. Prescription of QT-prolonging drugs in a cohort of about 5 million outpatients. Am J Med. 2003;114(2):135–41.
Das B, et al. Frequency, characteristics and nature of risk factors associated with use of QT interval prolonging medications and related drug-drug interactions in a cohort of psychiatry patients. Therapie. 2019;74(6):599–609.
Christensen L, et al. Identification of risk of QT prolongation by pharmacists when conducting medication reviews in residential aged care settings: a missed opportunity? J Clin Med. 2019;8(11).
Zarowitz BJ, Tisdale JE. Navigating the minefield of QTc interval-prolonging therapy in nursing facility residents. J Am Geriatr Soc. 2019;67(7):1508–15.
Svennberg E, et al. How to use digital devices to detect and manage arrhythmias: an EHRA practical guide. EP Europace; 2022:euac038.
Sharma S, et al. Providers’ response to clinical decision support for QT prolonging drugs. J Med Syst. 2017;41(10):161.
Tisdale JE, et al. Effectiveness of a clinical decision support system for reducing the risk of QT interval prolongation in hospitalized patients. Circ Cardiovasc Qual Outcomes. 2014;7(3):381–90.
Berger FA, et al. Development and validation of a tool to assess the risk of QT drug-drug interactions in clinical practice. BMC Med Inform Decis Mak. 2020;20(1):171.
Choi BJ, et al. Data-driven drug-induced QT prolongation surveillance using adverse reaction signals derived from 12-lead and continuous electrocardiogram data. PLoS One. 2022;17(1): e0263117.
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Putnikovic, M., Jordan, Z., Munn, Z. et al. Use of Electrocardiogram Monitoring in Adult Patients Taking High-Risk QT Interval Prolonging Medicines in Clinical Practice: Systematic Review and Meta-analysis. Drug Saf 45, 1037–1048 (2022). https://doi.org/10.1007/s40264-022-01215-x
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DOI: https://doi.org/10.1007/s40264-022-01215-x