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Screening for participants in the ISCHEMIA trial: Implications for clinical research

Published online by Cambridge University Press:  13 July 2022

Fatima Rodriguez Open the ORCID record for Fatima Rodriguez [Opens in a new window] ,
Judith S. Hochman ,
Yifan Xu ,
Harmony R. Reynolds ,
Jeffrey S. Berger ,
Stavroula Mavromichalis ,
Jonathan D. Newman ,
Sripal Bangalore  and
David J. Maron
Fatima Rodriguez*
Affiliation:
Division of Cardiovascular Medicine and the Cardiovascular Institute, Stanford University, Stanford, CA, USA Stanford Prevention Research Center, Department of Medicine, Stanford University, School of Medicine, Stanford, CA, USA
Judith S. Hochman
Affiliation:
New York University, Grossman School of Medicine, New York, NY, USA
Yifan Xu
Affiliation:
New York University, Grossman School of Medicine, New York, NY, USA
Harmony R. Reynolds
Affiliation:
New York University, Grossman School of Medicine, New York, NY, USA
Jeffrey S. Berger
Affiliation:
New York University, Grossman School of Medicine, New York, NY, USA
Stavroula Mavromichalis
Affiliation:
New York University, Grossman School of Medicine, New York, NY, USA
Jonathan D. Newman
Affiliation:
New York University, Grossman School of Medicine, New York, NY, USA
Sripal Bangalore
Affiliation:
New York University, Grossman School of Medicine, New York, NY, USA
David J. Maron
Affiliation:
Division of Cardiovascular Medicine and the Cardiovascular Institute, Stanford University, Stanford, CA, USA Stanford Prevention Research Center, Department of Medicine, Stanford University, School of Medicine, Stanford, CA, USA
*
Address for correspondence: F. Rodriguez, MD, MPH, FACC, FAHA, Assistant Professor, Stanford University, Center for Academic Medicine, 453 Quarry Road, Palo Alto, CA 94304, USA. Email: frodrigu@stanford.edu
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Abstract

The International Study of Comparative Health Effectiveness with Medical and Invasive Approaches (ISCHEMIA) found that there was no statistical difference in cardiovascular events with an initial invasive strategy as compared with an initial conservative strategy of guideline-directed medical therapy for patients with moderate to severe ischemia on noninvasive testing. In this study, we describe the reasons that potentially eligible patients who were screened for participation in the ISCHEMIA trial did not advance to enrollment, the step prior to randomization. Of those who preliminarily met clinical inclusion criteria on screening logs submitted during the enrollment period, over half did not participate due to physician or patient refusal, a potentially modifiable barrier. This analysis highlights the importance of physician equipoise when advising patients about participation in randomized controlled trials.

Keywords

Clinical trialsdisparitiesenrollmentscreeningstable ischemic heart disease
Type
Brief Report
Information
Journal of Clinical and Translational Science , Volume 6 , Issue 1 , 2022 , e90
Creative Commons
Creative Common License - CCCreative Common License - BY
This is an Open Access article, distributed under the terms of the Creative Commons Attribution licence (https://creativecommons.org/licenses/by/4.0/), which permits unrestricted re-use, distribution, and reproduction in any medium, provided the original work is properly cited.
Copyright
© The Author(s), 2022. Published by Cambridge University Press on behalf of The Association for Clinical and Translational Science

Participant recruitment in randomized controlled trials is often a challenge in terms of the time and cost required to complete a trial and the representativeness of the sample that is included. The objective of this report is to describe the reasons that potentially eligible participants who were screened did not advance to enrollment, the step prior to randomization in the International Study of Comparative Health Effectiveness with Medical and Invasive Approaches (ISCHEMIA) [Reference Maron, Hochman and Reynolds1].

Table 1. Characteristics of patients screened for the ISCHEMIA trial

* Other patients were excluded for reasons including not enough clinical information to determine if subject was suitable for inclusion (n = 496), could not be contacted (n = 513), went straight to angiography (n = 526), opted for medical therapy (n = 10), ischemia not verified by adjudication (n = 19), and unknown reasons (n = 3888).

A total of 182 patients screened were missing sex information.

The ISCHEMIA trial compared an initial invasive stragegy added to guideline-directed medical therapy with a conservative management strategy of guideline-directed medical therapy alone in patients with stable ischemic heart disease with significant ischemia. Patients with stable ischemic heart disease were selected for enrollment based on local site interpretation of moderate or severe ischemia on noninvasive stress testing [Reference Maron and Hochman2]. Key clinical exclusion criteria were recent acute coronary syndrome, unprotected left main stenosis of at least 50%, left ventricular systolic function <35%, New York Heart Association Class III or IV heart failure, estimated glomerular filtration rate (eGFR) <30 ml/min, or unacceptable angina despite maximal medical therapy. Eligible patients who consented for enrollment were randomized to an initial invasive strategy (n = 2,588) versus an initial conservative strategy (n = 2,591). Almost a quarter of those randomized were women (23%). After a median follow-up of 3.2 years, an initial invasive strategy did not reduce major adverse cardiovascular events as compared with initial conservative management (13.3% vs. 15.5%, P = 0.34), although patients with angina at baseline assigned to the invasive strategy had greater improvement in quality of life [Reference Maron, Hochman and Reynolds1, Reference Spertus, Jones and Maron3].

Methods

Potential participants were identified and recruited from stress testing laboratories. The ischemia eligibility criteria were at least moderate ischemia on a stress imaging test or severe ischemia on a non-imaging exercise tolerance test as defined by the protocol and interpreted by the site.

From January 2012 to February 2018, we asked sites to complete screening logs of consecutive patients who underwent stress testing and met ischemia eligibility criteria and to submit them to the Clinical Coordinating Center (CCC) every month. This activity was not funded, and sites were not required to submit logs over this entire period. Sites that enrolled at least one participant per month over the previous 3 months were not asked to submit screening logs. The information provided on the log included the total number of stress tests performed in the past month at the site’s primary stress laboratory. Data entered for patients who met ischemia eligibility criteria were age, sex, and whether the patient provided consent or was excluded due to meeting an exclusion criterion, along with the reason for exclusion. Refusal by the patient or the patient’s physician was also documented, but not the reason for such refusal. As of January 1, 2017, submission of screening logs to the CCC became optional for all sites.

This analysis includes patients entered on screening logs for which information about clinical eligibility was available. We computed descriptive statistics as frequencies and percentages for categorical variables and medians and interquartile ranges for continuously measured variables.

Results

A total of 380 sites in 38 countries were eligible to screen and enroll participants. Among these, 339 sites enrolled participants and 308 sites (81%) submitted screening logs. A total of 4,014 screening logs collected from 308 sites between January 2012 and February 2018 (22,792 site months) were considered in this analysis, with a total of 28,324 patients entered. We excluded 1,987 patients for whom the reason for exclusion was not documented, 75 patients from sites only enrolling in ISCHEMIA-Chronic Kidney Disease, and 8 with input errors, yielding a sample of 26,254 patients with moderate or severe ischemia on stress testing. Of these, a total of 12,325 met protocol-defined clinical exclusion criteria and 2,766 were consented and enrolled (Table 1). Among the remaining 11,163 apparently clinically eligible but excluded patients, 3,039 (27.2%) were excluded due to physician refusal, 2,672 (23.9%) were excluded due to patient refusal, and 5,452 were excluded for various other reasons. Sites reported that some patients were excluded due to difficulty with patient contact (n = 513, 4.6%) or referral to angiography before consent could be obtained (n = 526, 4.7%). Few patients (n = 43, 0.2% of those screened) with eGFR between 30 and 59 ml/min were excluded because of physician suspicion of unprotected left main disease. Of all women screened, 9.4% were consented for trial enrollment compared with 11.1% of all men. A more pronounced sex difference was observed among those in this sample who appeared clinically eligible at screening who subsequently agreed to participate in the trial: 17.2% of women consented versus 21.1% of men (P < 0.001).

Participants from study sites located in Asia were more likely to consent for trial enrollment (39.4%), whereas those from North America were least likely to enroll (10.5%). Among clinically eligible patients who were excluded, patient refusal was highest in Other regions (23.9%) and lowest in Latin America (13.1%). Physician refusal was highest in North America (27.2%) and lowest in Asia (9.4%).

Discussion

In this analysis, we report the rates of physician and patient refusal for trial enrollment within a sample of patients who were screened for ISCHEMIA based on moderate or severe ischemia on stress testing. Of those who apparently met clinical inclusion criteria on preliminary screening, over half did not participate due to physician or patient refusal. This rate of physician and patient refusal was disappointing and illustrates an important challenge to recruiting patients to participate in clinical trials. When there is uncertainty about the efficacy of an intervention, the best method to establish evidence is to conduct a randomized controlled trial. Physicians must have equipoise when optimal management is uncertain and explain to patients that there is a gap in evidence to define optimal management of their condition. Indeed, one could question the ethics of practicing without evidence or preventing a patient from being informed about or participating in a clinical trial when there is uncertainty regarding the best management strategy. In the case of ISCHEMIA, despite community equipoise whether revascularization reduces clinical event rates in patients with stable ischemic heart disease [Reference Stone, Hochman and Williams4], we encountered challenges to enrolling apparently eligible patients with moderate or severe ischemia into a trial with a 50% chance of being randomized to a conservative (i.e., non-revascularization) management strategy. These decisions are undoubtedly influenced by preexisting patient and physician beliefs regarding the risks and benefits of the treatment strategies tested. Notably, sites in the North American region had the lowest rates of enrollment and were more likely to have physicans refuse study participation than other study regions.

Data show that women are less likely to undergo stress testing, a phenomenon in part attributable to implicit sex bias of cardiologists [Reference Daugherty, Blair and Havranek5]. ISCHEMIA also found that women who were screened for study participation were less likely to consent as compared with men, with sex-based disparities more pronounced among clinically eligible participants [Reference Reynolds, Shaw and Min6]. This suggests that the observed sex-specific disparities are not fully explained by differences in the prevalence of obstructive coronary disease between men and women with similar degrees of ischemia. Female sex has been associated with lower clinical trial participation rates in other cardiovascular and stroke randomized trials, threatening the generalizability of study results [Reference Martin, Ou and Newby7, Reference O’Neill, Deptuck and Quong8]. Similar to our study that documents that women were more likely to decline study participation, one study found that women were 15% less willing to participate in cardiovascular disease prevention trials, perceiving a greater chance of harm than benefit from trial participation [Reference Ding, Powe, Manson, Sherber and Braunstein9]. Given the high burden of cardiovascular morbidity and mortality in women, increasing representation of women in practice-informing clinical trials is of paramount importance. Analyses from ISCHEMIA have already demonstrated sex differences between participants in terms of angina severity, anatomic severity of disease, degree of ischemia, and risk factor control [Reference Reynolds, Shaw and Min6, Reference Newman, Alexander and Gu10].

A limitation of this study is that the screening log sample does not reflect all patients screened, enrolled, and randomized into the trial. Screening logs were completed intermittently at only 81% of enrolling sites and were skewed toward lower enrolling sites in line with the purpose of screening logs as a tool to assess and act upon enrollment challenges. Two-thirds of those screened in this cohort had clinical exclusion criteria. The screening log did not assess race, ischemia severity (moderate vs. severe), angina severity, the reasons for physician and patient refusal, or clinical outcomes for excluded patients. The proportion of patient and physician refusals is subject to uncertainty as the assessment of clinical eligibility was preliminary, for example, details were not pursued further if there was a refusal. It is possible that the reasons for refusal could have biased the sample in way that affected trial results.

In conclusion, analyses from screening logs from ISCHEMIA, submitted by sites over varying durations of the enrollment period, demonstrate that two-thirds of patients screened had a clinical exclusion criterion. Among apparently eligible patients excluded from trial enrollment, patient and physician refusal accounted for over half of exclusions, and women were less likely than men to agree to participate. These findings underscore the importance of physician equipoise when advising patients about participation in randomized controlled trials. More work is also needed to dismantle reasons for sex-based differences in cardiovascular clinical trial participation.

Acknowledgements

The authors would like to thank the ISCHEMIA study participants and participating study sites. NIH grants U01HL105907, U01HL105462, U01HL105561, and U01HL105565.

Disclosures

Dr. Fatima Rodriguez was funded by a career development award from the National Heart, Lung, and Blood Institute (K01 HL 144,607), the American Heart Association/Robert Wood Johnson Harold Amos Medical Faculty Development Program, and grant #2022051 from the Doris Duke Charitable Foundation. Outside the submitted work, Dr. Rodriguez reports equity from HealthPals and consulting fees from Novartis and clinical event adjudication for NovoNordisk. Dr. Judith S. Hochman is PI for the ISCHEMIA trial for which, in addition to support by National Heart, Lung, and Blood Institute grant, devices and medications were provided by Abbott Vascular; Medtronic, Inc.; Abbott Laboratories (formerly St. Jude Medical, Inc); Royal Philips NV (formerly Volcano Corporation); Arbor Pharmaceuticals, LLC; AstraZeneca Pharmaceuticals, LP; Merck Sharp & Dohme Corp.; Omron Healthcare, Inc, Sunovion Pharmaceuticals, Inc. Espero BioPharma; and Amgen, Inc; and financial donations from Arbor Pharmaceuticals LLC and AstraZeneca Pharmaceuticals LP. Yifan Xu reports grants from National Heart, Lung, and Blood Institute during the conduct of the study. Dr. Harmony R. Reynolds reports grants from National Heart, Lung, and Blood Institute during the conduct of the study; nonfinancial support from Abbott Vascular, nonfinancial support from Siemens, nonfinancial support from BioTelemetry, outside the submitted work. Dr. Jeffrey S. Berger reports grants from National Heart, Lung, and Blood Institute during the conduct of the study. Stavroula Mavromichalis reports grants from National Heart, Lung, and Blood Institute during the conduct of the study. Dr. Jonathan D. Newman reports grants from National Heart, Lung, and Blood Institute during the conduct of the study. Dr. Sripal Bangalore reports grants from National Heart, Lung, and Blood Institute, during the conduct of the study; grants and personal fees from Abbott Vascular, personal fees from Biotronik, Pfizer, Amgen, and Reata outside the submitted work. Dr. David J. Maron reports grants from National Heart, Lung, and Blood Institute during the conduct of the study.

References

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Figure 0

Table 1. Characteristics of patients screened for the ISCHEMIA trial