Publication

• Title: Emergency vs Delayed Coronary Angiogram in Survivors of Out-of-Hospital Cardiac Arrest: Results of the Randomized, Multicentric EMERGE Trial
• Acronym: EMERGE
• Year: 2022
• Journal published in: JAMA Cardiology
• Citation: Hauw-Berlemont C, Lamhaut L, Diehl JL, et al; EMERGE Trial Investigators. Emergency vs delayed coronary angiogram in survivors of out-of-hospital cardiac arrest: results of the randomized, multicentric EMERGE trial. JAMA Cardiol. 2022;7(7):700-707.

Context & Rationale

• Background

  • Out-of-hospital cardiac arrest (OHCA) survivors without ST-segment elevation can still have an acute coronary culprit lesion, but post-return of spontaneous circulation (ROSC) ECG has imperfect sensitivity for acute coronary occlusion.
  • Observational registries and early invasive “cardiac arrest centre” pathways supported early coronary angiography (CAG) and percutaneous coronary intervention (PCI) as potentially time-critical and modifiable contributors to outcome.
  • Competing priorities in early post-arrest care include haemodynamic stabilisation, ventilation, temperature management, and neuroprognostication; routine emergency CAG could delay ICU-based care, add iatrogenic risk, and consume system resources.
  • Before EMERGE, equipoise persisted regarding whether a routine “go-to-cath-lab” strategy improves patient-centred outcomes in OHCA without ST-elevation, as opposed to a selective or delayed approach.
• Research Question/Hypothesis

  • Whether an emergency CAG strategy is superior to a delayed CAG strategy (48–96 hours) for improving 180-day survival free of major neurological sequelae in OHCA survivors without ST-segment elevation and without an obvious non-cardiac cause.
• Why This Matters

  • Routine emergency CAG is a high-resource, high-consequence pathway that drives prehospital triage and hospital system design.
  • Demonstrating benefit would justify system-wide cath-lab activation and early invasive treatment for a broad OHCA cohort; demonstrating no benefit would support an ICU-first, selective invasive strategy.
  • Neurologically intact survival is the outcome that matters to patients and families, and it is plausibly affected by both early coronary reperfusion (if indicated) and uninterrupted high-quality post-resuscitation ICU care.

Design & Methods

• Research Question: In adult survivors of OHCA without ST-segment elevation and without an obvious non-cardiac cause, does an emergency coronary angiography strategy (vs delayed coronary angiography at 48–96 hours) improve 180-day survival free of major neurological sequelae?
• Study Type: Investigator-initiated, multicentre, open-label, randomised, parallel-group, superiority trial; national (France); randomisation in the prehospital/early hospital phase; intervention in the cardiac catheterisation laboratory; post-resuscitation care in ICU.
• Population:
  • Adults (≥18 years) with out-of-hospital sudden cardiac arrest and sustained ROSC.
  • No obvious non-cardiac cause identified at presentation (eg, trauma/neurological/respiratory cause).
  • Absence of ischaemic ST-segment elevation on the post-ROSC ECG (left bundle branch block was not treated as a STEMI equivalent for inclusion).
  • Admitted to a centre with ICU capability and 24/7 interventional cardiology service.
  • Key exclusions: in-hospital cardiac arrest; no ROSC; ischaemic ST-segment elevation; suspected non-cardiac aetiology; major comorbidity with life expectancy <1 year; pregnancy; legal protection status; participation in another interventional trial.
  • Deferred consent framework: patients could be excluded post-randomisation if consent could not be obtained (per trial flow diagram).
  • Randomisation stratified by pre-specified prognostic strata: “Group 1” required all of age <75 years, initial shockable rhythm, no-flow <5 minutes, low-flow <20 minutes, and epinephrine dose <1 mg; “Group 2” otherwise.
• Intervention:
  • Emergency coronary angiography strategy with immediate transfer to the cardiac catheterisation laboratory as soon as feasible after admission.
  • PCI performed during the index procedure when an angiographic culprit lesion was identified, consistent with contemporary invasive coronary treatment strategies for OHCA survivors.
  • Post-resuscitation ICU care otherwise delivered according to local practice (eg, temperature management, ventilatory/haemodynamic support).
• Comparison:
  • Delayed coronary angiography strategy planned for 48–96 hours after ICU admission.
  • Urgent coronary angiography before the planned window permitted when clinically indicated (eg, deterioration or suspected ongoing coronary ischaemia), at treating team discretion.
  • Post-resuscitation ICU care according to local practice, as per the intervention group.
• Blinding: Open-label for clinicians and sites; primary endpoint assessed by an independent physician masked to randomisation allocation.
• Statistics: Planned total sample size 970 to detect a 10% absolute improvement in the primary endpoint (from 36% to 46%) with 80% power at a two-sided 5% significance level (allowing for 30% crossover and 10% loss to follow-up); primary analysis by intention-to-treat with time-to-event methods (Kaplan–Meier/log-rank; Cox proportional hazards models adjusted for stratification group and accounting for centre effects).
• Follow-Up Period: 180 days (with additional neurological outcome ascertainment at ICU discharge and 90 days).

Key Results

This trial was stopped early. Recruitment ceased after funding termination when a prespecified recruitment-rate threshold was not reached; 279 patients were included in analyses (planned 970).

Outcome	Emergency CAG strategy	Delayed CAG strategy	Effect	p value / 95% CI	Notes
Primary: 180-day survival free of major neurological sequelae (CPC 1–2)	47/141 (34.1%)	42/138 (30.7%)	HR 0.87	95% CI 0.65 to 1.15; P=0.32	Time-to-event analysis; major neurological sequelae defined as CPC 3–5
180-day survival	51/141 (36.2%)	46/138 (33.3%)	HR 0.86	95% CI 0.64 to 1.15; P=0.31	No between-group difference detected
Coronary angiography performed	126/141 (89.4%)	74/138 (53.6%)	Not reported	Not reported	In the delayed group, 23/74 (31.1%) underwent “urgent” angiography before the planned 48–96 h window
Time from OHCA to coronary angiography, median (IQR), hours	2 (2 to 3)	65.5 (40.8 to 74.8)	Not reported	Not reported	Demonstrates protocol separation in timing of angiography
Shock during first 48 hours	50/129 (38.8%)	53/133 (39.8%)	RR 1.03	95% CI 0.76 to 1.39; P=0.86	Risk ratio reported in trial table; definition as per protocol
Ventricular tachycardia/ventricular fibrillation during first 48 hours	10/141 (7.1%)	5/138 (3.6%)	RR 0.51	95% CI 0.18 to 1.46; P=0.21	No statistically significant difference
Withdrawal of life-sustaining care	56/141 (39.7%)	65/138 (47.1%)	RR 1.19	95% CI 0.91 to 1.55; P=0.22	Potentially important competing pathway for outcome; no between-group difference detected

• Emergency CAG did not improve 180-day survival with favourable neurological outcome: 34.1% vs 30.7% (HR 0.87; 95% CI 0.65 to 1.15; P=0.32).
• There was large separation in angiography timing (median 2 hours vs 65.5 hours), yet no signal of improved patient-centred outcomes in the analysed sample.
• Early stopping meant substantially reduced statistical power versus the planned sample size, limiting precision around clinically important effect sizes.

Internal Validity

• Randomisation and Allocation:
  • Centralised, web-based 1:1 randomisation with variable block sizes; allocation sequence generated in advance and held by the sponsor.
  • Randomisation performed by an emergency physician at the dispatch centre (independent of recruiting clinicians), or within 1 hour of admission if not randomised prehospital.
  • Stratification by a prognostic stratum (Group 1 vs Group 2) based on age, initial rhythm, no-flow/low-flow times, and epinephrine dose.
• Drop out or exclusions:
  • 338 patients were randomised; 59 (17.5%) were excluded after randomisation (37 lacked consent; 16 did not meet inclusion criteria; 6 other reasons), leaving 279 in the analysed cohort.
  • Deferred consent with post-randomisation exclusion introduces the possibility of selection after allocation, and represents a departure from a strict intention-to-treat principle.
  • Follow-up attrition at 180 days was low but present (patients lost to follow-up or declining follow-up were reported in the participant flow diagram); primary analysis used time-to-event methods with censoring.
• Performance/Detection Bias:
  • Open-label allocation could influence co-interventions (eg, haemodynamic support decisions, timing of neuroprognostication) and clinician behaviour.
  • Primary endpoint was assessed by an independent physician masked to allocation, mitigating detection bias for neurological outcome classification.
• Protocol Adherence:
  • Emergency group: coronary angiography performed in 126/141 (89.4%); 15/141 (10.6%) did not undergo angiography.
  • Delayed group: coronary angiography performed in 74/138 (53.6%); 23/74 (31.1%) underwent angiography earlier than the planned window; 64/138 (46.4%) had no angiography.
  • PCI among those undergoing angiography: 38/126 (30.2%) vs 17/74 (23.0%).
• Baseline Characteristics:
  • Groups were broadly similar: mean age 65.4 (13.1) vs 63.9 (12.7) years; male sex 103/141 (73.1%) vs 92/138 (66.7%).
  • Initial rhythm was predominantly non-shockable: 92/141 (65.2%) vs 96/138 (69.9%).
  • Post-resuscitation coma severity was similar: Glasgow Coma Scale median 3 (IQR 3–3) in both groups.
  • Targeted temperature management use was similar: 73/141 (52.0%) vs 74/138 (53.7%).
• Heterogeneity:
  • Multicentre design increases clinical heterogeneity in ICU and cath-lab practice; analyses accounted for centre effects in modelling.
  • Case-mix included shockable and non-shockable rhythms and a substantial burden of non-coronary precipitants that were not “obvious” at enrolment, reflecting pragmatic enrolment but also diluting a potential coronary-specific treatment effect.
• Timing:
  • Separation in timing was achieved: time from OHCA to angiography median 2 (2 to 3) hours vs 65.5 (40.8 to 74.8) hours.
  • Mean delay from randomisation to angiography was 0.6 (3.7) hours vs 55.1 (37.2) hours.
• Dose:
  • The “dose” of invasive management, in terms of angiography completion and revascularisation, differed less than timing alone might suggest because many delayed-strategy patients died before angiography and a subset underwent urgent early angiography.
  • No significant coronary disease was common among those catheterised: 57/126 (45.2%) vs 41/74 (55.4%).
• Separation of the Variable of Interest:
  • Angiography exposure: 126/141 (89.4%) vs 74/138 (53.6%).
  • Timing exposure: 2 (2 to 3) hours vs 65.5 (40.8 to 74.8) hours from arrest to angiography.
  • Strategy contamination: “urgent” angiography occurred in 23/138 delayed-strategy patients (performed within 14.7 hours), with 7 undergoing intervention.
• Key Delivery Aspects:
  • Enrolment occurred early (prehospital or within 1 hour of admission), which is appropriate for testing an early cath-lab pathway.
  • Control strategy was an explicit delayed pathway (48–96 hours) rather than an uncontrolled “usual care” approach, improving interpretability.
• Outcome Assessment:
  • Primary endpoint was clinically meaningful (neurologically intact survival) and assessed at 180 days.
  • Cerebral Performance Category is a standard post-arrest measure but remains partly subjective; masking of assessors mitigates (but does not eliminate) classification variability.
• Statistical Rigor:
  • Time-to-event analysis with pre-specified covariate adjustment was appropriate for the endpoint definition.
  • Early stopping substantially reduced the ability to exclude clinically important effects, and the wide confidence intervals reflect imprecision.

Conclusion on Internal Validity: Overall, internal validity appears moderate: randomisation and timing separation were strong, and outcome assessment was masked, but early stopping, substantial post-randomisation exclusions related to consent/eligibility, and meaningful protocol non-adherence in the delayed group reduce precision and raise residual bias concerns.

External Validity

• Population Representativeness:
  • Includes a pragmatic OHCA cohort without ST-elevation, with a majority presenting with non-shockable rhythms, which mirrors many real-world OHCA case-mixes in contemporary systems.
  • Enrolment required admission to centres with 24/7 interventional cardiology and ICU capability, which may select for higher-resource systems and structured regional pathways.
• Applicability:
  • Findings apply to OHCA survivors without ST-elevation and without an obvious non-cardiac cause; they do not address patients with ST-elevation (where emergency angiography is standard).
  • In systems with limited cath-lab access, results support that a delayed/selective approach may be acceptable for many stable post-arrest patients without ST-elevation, provided urgent angiography remains available when clinically indicated.
  • Generalisation to pathways with different neuroprognostication practices, withdrawal-of-care norms, or post-arrest ICU bundles should be made cautiously.

Conclusion on External Validity: Generalisability is moderate: the OHCA population is clinically representative, but applicability is strongest in systems able to deliver both rapid ICU care and selective/urgent cath-lab access within a structured regional network.

Strengths & Limitations

• Strengths:
  • Randomised design addressing a high-impact systems-of-care question in OHCA without ST-elevation.
  • Clinically meaningful primary endpoint prioritising neurological outcome at 180 days.
  • Early randomisation (prehospital/early hospital) testing the real-world cath-lab pathway decision point.
  • Masked endpoint assessment by an independent physician.
  • Substantial achieved separation in angiography timing (median 2 hours vs 65.5 hours).
• Limitations:
  • Early stopping with marked under-recruitment versus the planned sample size, resulting in reduced power and imprecision.
  • Post-randomisation exclusions for deferred consent/eligibility, deviating from strict intention-to-treat principles.
  • Open-label intervention with potential co-intervention and care-pathway effects.
  • Protocol non-adherence and contamination in the delayed group: only 53.6% underwent angiography, and 23 patients underwent “urgent” early angiography.
  • High competing risk of death from neurological injury limits the proportion of patients for whom coronary revascularisation can plausibly be outcome-modifying.

Interpretation & Why It Matters

• Clinical practice

  • A routine emergency angiography strategy did not improve neurologically intact survival compared with a delayed (48–96 h) strategy in this OHCA cohort without ST-elevation.
  • These data support an ICU-first, selective invasive strategy in many patients, while preserving urgent angiography for evolving clinical indications.
• Trialist/methodologist lens

  • The pragmatic case-mix increases relevance but likely dilutes a coronary-specific treatment effect in a population where neurological injury dominates outcome.
  • Deferred consent and early stopping are pivotal design/operational constraints in emergency care trials that meaningfully shape interpretability and precision.
• What’s next

  • Future work should sharpen selection for potentially reversible coronary occlusion (eg, physiology, imaging, biomarkers, refined ECG timing) rather than broad routine cath-lab activation.
  • Systems research should integrate patient-centred outcomes and competing risks (withdrawal-of-care practices, neuroprognostication) into pathway evaluation.

Controversies & Subsequent Evidence

• Precision and interpretability after early stopping:
  • Stopping far short of the planned sample size limits the ability to rule in or rule out clinically important benefit or harm, despite point estimates close to neutrality.
• Deferred consent and post-randomisation exclusions:
  • Excluding 59 randomised participants after allocation (notably for lack of consent) creates a “modified ITT” cohort and can introduce selection bias if exclusions differ by prognosis or pathway effects.
• Contamination of the control strategy:
  • The delayed strategy included both “no angiography” (often due to early death) and “urgent early angiography” (23 patients), complicating causal attribution to timing alone.
• How EMERGE aligns with other randomised evidence:
  • Other randomised trials in OHCA without ST-elevation also reported no improvement in key outcomes with routine immediate angiography strategies (COACT, PEARL, TOMAHAWK).¹²³
• Tension between earlier observational support and trial results:
  • Consensus and registry-driven pathways historically supported early invasive management after OHCA, based on perceived prevalence of treatable culprit lesions and observational survival associations.⁴⁵
  • EMERGE’s angiographic findings reinforce the challenge of case selection: nearly half of catheterised patients had no significant coronary disease, and PCI occurred in 30.2% vs 23.0% among those undergoing angiography.

Summary

• In OHCA survivors without ST-elevation and without an obvious non-cardiac cause, an emergency angiography strategy did not improve 180-day survival free of major neurological sequelae compared with a delayed (48–96 h) strategy.
• The trial stopped early for funding/recruitment reasons, enrolling 279 of a planned 970 participants, limiting statistical power and precision.
• Separation in angiography timing was substantial (median 2 hours vs 65.5 hours), yet patient-centred outcomes were similar.
• Protocol adherence differed: angiography was performed in 89.4% vs 53.6%, and urgent early angiography occurred in a subset of delayed-strategy patients.
• Findings support an ICU-first approach with selective/urgent angiography when clinically indicated, rather than routine immediate angiography for all such patients.

Further Reading

Other Trials

• 2019Lemkes JS, Janssens GN, van der Hoeven NW, et al. Coronary angiography after cardiac arrest without ST-segment elevation. N Engl J Med. 2019;380(15):1397-1407.
• 2020Kern KB, Radsel P, Jentzer JC, et al. Randomized pilot clinical trial of early coronary angiography versus no early coronary angiography after cardiac arrest without ST-segment elevation: the PEARL study. Circulation. 2020;142(21):2002-2012.
• 2021Desch S, Freund A, Akin I, et al. Angiography after out-of-hospital cardiac arrest without ST-segment elevation. N Engl J Med. 2021;385(27):2544-2553.
• 2006Hochman JS, Sleeper LA, Webb JG, et al. Early revascularization and long-term survival in cardiogenic shock complicating acute myocardial infarction. JAMA. 2006;295(21):2511-2515.

Systematic Review & Meta Analysis

• 2010Sasson C, Rogers MAM, Dahl J, Kellermann AL. Predictors of survival from out-of-hospital cardiac arrest: a systematic review and meta-analysis. Circ Cardiovasc Qual Outcomes. 2010;3(1):63-81.
• 2012Larsen JM, Ravkilde J. Acute coronary angiography in patients resuscitated from out-of-hospital cardiac arrest: a systematic review and meta-analysis. Resuscitation. 2012;83(12):1427-1433.
• 2018Mayet A, Song KJ, Rea T. Out-of-hospital cardiac arrest: current concepts. Lancet. 2018;391(10124):970-979.
• 2012Deo R, Albert CM. Epidemiology and genetics of sudden cardiac death. Circulation. 2012;125(4):620-637.

Observational Studies

• 1997Spaulding CM, Joly LM, Rosenberg A, et al. Immediate coronary angiography in survivors of out-of-hospital cardiac arrest. N Engl J Med. 1997;336(23):1629-1633.
• 2010Dumas F, Cariou A, Manzo-Silberman S, et al. Immediate percutaneous coronary intervention is associated with better survival after out-of-hospital cardiac arrest: insights from the PROCAT registry. Circ Cardiovasc Interv. 2010;3(3):200-207.
• 2016Dumas F, Bougouin W, Geri G, et al. Emergency percutaneous coronary intervention in post-cardiac arrest patients without ST-segment elevation pattern: insights from the PROCAT II registry. JACC Cardiovasc Interv. 2016;9(10):1011-1018.
• 2021Baldi E, Schnaubelt S, Caputo ML, et al. Association of timing of electrocardiogram acquisition after return of spontaneous circulation with coronary angiography findings in patients with out-of-hospital cardiac arrest without ST-segment elevation. JAMA Netw Open. 2021;4(1):e20232875.
• 2011Sideris G, Voicu S, Dillinger JG, et al. Value of postresuscitation electrocardiogram in the diagnosis of acute myocardial infarction in out-of-hospital cardiac arrest patients. Resuscitation. 2011;82(9):1148-1153.

Guidelines

• 2014Noc M, Fajadet J, Lassen JF, et al. Invasive coronary treatment strategies for out-of-hospital cardiac arrest: a consensus statement from the European Association for Percutaneous Cardiovascular Interventions (EAPCI)/Stent for Life groups. EuroIntervention. 2014;10(1):31-37.
• 2014Windecker S, Kolh P, Alfonso F, et al. 2014 ESC/EACTS guidelines on myocardial revascularization. Eur Heart J. 2014;35(37):2541-2619.
• 2018Ibanez B, James S, Agewall S, et al. 2017 ESC guidelines for the management of acute myocardial infarction in patients presenting with ST-segment elevation. Eur Heart J. 2018;39(2):119-177.
• 2020Kiguchi T, Okubo M, Nishiyama C, et al. Out-of-hospital cardiac arrest across the world: first report from the International Liaison Committee on Resuscitation (ILCOR). Resuscitation. 2020;152:39-49.

Notes

• Where risk ratios are presented, interpret direction in line with the original trial tables; no additional calculations were performed for this summary.

Overall Takeaway

EMERGE tested a systems-defining question in post-cardiac arrest care: whether routine emergency coronary angiography improves neurologically intact survival in OHCA survivors without ST-elevation. Despite substantial separation in angiography timing, the trial found no improvement in 180-day neurological outcome or survival, and early stopping with non-adherence limits precision rather than reversing the overall message. In the context of concordant randomised evidence, EMERGE supports an ICU-first, selective invasive strategy for many such patients, reserving urgent coronary angiography for evolving clinical indications.

Bibliography

• 1Lemkes JS, Janssens GN, van der Hoeven NW, et al. Coronary angiography after cardiac arrest without ST-segment elevation. N Engl J Med. 2019;380(15):1397-1407.
• 2Kern KB, Radsel P, Jentzer JC, et al. Randomized pilot clinical trial of early coronary angiography versus no early coronary angiography after cardiac arrest without ST-segment elevation: the PEARL study. Circulation. 2020;142(21):2002-2012.
• 3Desch S, Freund A, Akin I, et al. Angiography after out-of-hospital cardiac arrest without ST-segment elevation. N Engl J Med. 2021;385(27):2544-2553.
• 4Noc M, Fajadet J, Lassen JF, et al. Invasive coronary treatment strategies for out-of-hospital cardiac arrest: a consensus statement from the European Association for Percutaneous Cardiovascular Interventions (EAPCI)/Stent for Life groups. EuroIntervention. 2014;10(1):31-37.
• 5Dumas F, Bougouin W, Geri G, et al. Emergency percutaneous coronary intervention in post-cardiac arrest patients without ST-segment elevation pattern: insights from the PROCAT II registry. JACC Cardiovasc Interv. 2016;9(10):1011-1018.