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Clinical Trial Details — Status: Terminated

Administrative data

NCT number NCT03707314
Other study ID # EDGE 89678
Secondary ID
Status Terminated
Phase N/A
First received
Last updated
Start date November 6, 2018
Est. completion date October 28, 2021

Study information

Verified date November 2022
Source University Hospitals, Leicester
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

Prospective, open, multicentre, randomised controlled trial in patients with higher risk non-ST elevation myocardial infarction acute coronary syndrome


Description:

Background: Clinical event rates in Non ST elevation myocardial infarction acute coronary syndrome (N-STEMI ACS) patients remain high, with one year MACE rates as high as 20%. While there may be early mortality differences between N-STEMI and STEMI, outcomes beyond one year become very similar. N-STEMI ACS patients therefore rightly remain the focus of a number of research directives. The objective of the RAPID-NSTEMI trial is to determine if clinical outcomes can be improved by very early intervention in a pre-determined higher risk N-STEMI ACS population. Published data has shown that inpatient Percutaneous Coronary Intervention (PCI) in N-STEMI ACS patients reduces subsequent clinical events. This had led to guidelines supporting its use in clinical practice. However, there is much less certainty regarding the timing of the PCI and, in particular, whether this should be a strategy used early to optimize outcomes. Thus, while evidence based guidelines (NICE and European) provide general time parameters for PCI, immediate angiography with a view to intervention in higher risk patients has never been robustly tested in any adequately powered, prospective randomised trial with clinical end points. The RAPID-NSTEMI trial sets out to test the benefits, or otherwise, of a strategy of immediate angiography with follow-on revascularisation in higher risk N-STEMI ACS patients. Hypothesis: Very early angiography +/- PCI improves clinical outcomes in higher risk NSTEMI patients when compared to standard invasive management. Methods: In order to identify higher risk patients as soon as possible after presentation, a high sensitivity troponin (Hs-Troponin-T or Hs-Troponin-I) will be taken, allowing calculation of a GRACE 2.0 score (GS 2.0) early after admission. The GS 2.0 will be determined in sufficient time to be able to test an early intervention strategy arm. Patients with GS 2.0 of ≥118 alone, or ≥90 with additional high risk features will be randomised in a 1:1 fashion to one of two groups: Group A: immediate angiography with follow-on revascularisation if required Group B: standard care - pharmacological treatment until angiography with follow on revascularisation if required (preferably within 72 hours as per current guidelines). The primary outcome for the main study will be a 12-month of all-cause mortality, new myocardial infraction and hospital admission with heart failure. Power calculations indicate that 2314 patients are required to show MACE superiority for early intervention in such higher risk N-STEMI ACS patients. Analyses will be primarily according to "intention to treat", with a secondary analysis according to trial treatment received (comparing those who actually received follow-on revascularisation at the two different trial time points). There will be a cost effectiveness analysis. Mechanistic sub-studies in the two groups will be undertaken. 1. Cardiac magnetic resonance imaging substudy to assess differences in infarct size, oedema, microvascular obstruction and left ventricular ejection fraction between the two arms. 2. Novel biomarkers substudy that will be funded separately after appropriate funding applications Expected value of results: The investigators have designed a superiority trial to anticipate that outcomes will be improved in higher risk patients revascularised very early after presentation with N-STEMI. Irrespective of outcome, this trial should determine whether there is a need for a change in current patient management of a common condition and, in particular, if all N-STEMI patients should be admitted to a PCI-capable hospital to allow for very early intervention. The results will inform national and international guidelines. The planned cost effectiveness analysis will become particularly important if clinical outcomes are no different between groups since length of stay should be different.


Recruitment information / eligibility

Status Terminated
Enrollment 425
Est. completion date October 28, 2021
Est. primary completion date October 28, 2021
Accepts healthy volunteers No
Gender All
Age group 18 Years and older
Eligibility Inclusion Criteria - 18 years of age and over - Patients presenting to hospitals with a clinical diagnosis of non-ST elevation myocardial infarction comprising: - Ischaemic symptoms (as defined in Appendix III of protocol) - Elevated high sensitivity Troponin T or I (above the normal range for individual hospitals) - GRACE-2.0 score (www.gracescore.org) of either: - =118 (corresponding to 6-month death >6%) OR - =90 but <118 (corresponding to 6-month death >3% but <6%) - If GRACE 2.0 score =90 or <118 must have at least one additional high risk feature: - Anterior location of ECG changes (leads V2 - V5) - ST-segment depression in 2 contiguous leads (any territory) of 0.15mV/ 1.5mm. - Diabetes Mellitus on medication - High-sensitivity Troponin I or T 3 x ULN - Onset of ischaemic symptoms at any time prior to admission but most recent episode within 12 hours to admission - Intention to perform angiography and, if indicated, follow-on revascularisation - Provision of assent or written consent - Randomisation must be performed within 6 hours of admission Exclusion Criteria - ST elevation myocardial infarction - Evident type 2 myocardial infarction (e.g. anaemia) - Evidence of previous known cardiomyopathy - Cardiogenic Shock - Known severe valvular heart disease - Need for urgent PCI according to ESC Guidelines (haemodynamic instability, VT, VF, recurrent or persistent pain) - Any contraindication to PCI - Current participation in another intervention trial

Study Design


Related Conditions & MeSH terms


Intervention

Procedure:
Angiography with follow-on revascularisation if indicated
Angiography with follow-on revascularisation (if indicated)

Locations

Country Name City State
United Kingdom Glenfield Hospital, University Hospitals of Leicester NHS Trust Leicester

Sponsors (4)

Lead Sponsor Collaborator
University Hospitals, Leicester British Heart Foundation, University of East Anglia, University of Leicester

Country where clinical trial is conducted

United Kingdom, 

Outcome

Type Measure Description Time frame Safety issue
Primary Major adverse cardiovascular events Incidence of the composite of all-cause mortality, new myocardial infarction and admission for heart failure within 12 months following randomisation 12 months
Secondary All-cause mortality Incidence of all-cause mortality 12 months
Secondary New myocardial infarction Incidence of new myocardial infarction 12 months
Secondary Heart failure Incidence of admission for heart failure 12 months
Secondary Cardiovascular mortality Incidence of cardiovascular mortality 12 months
Secondary Length of in-patient stay Length of in-patient stay (defined as randomisation to first discharge) in days Through study completion, 3 years
Secondary All-cause mortality prior to planned coronary angiography Incidence of all-cause mortality prior to planned coronary angiography following index admission with NSTEMI During index admission
Secondary New myocardial infarction prior to planned coronary angiography Incidence of new myocardial infarction prior to planned coronary angiography following index admission with NSTEMI During index admission
Secondary Major bleeding prior to planned coronary angiography Incidence of major bleeding (classified as BARC 3-5) prior to planned coronary angiography following index admission with NSTEMI During index admission
Secondary Admission for ischaemia-driven revascularisation Incidence of admission for ischaemia-driven revascularisation 12 months
Secondary Admission for any cause Incidence of admission for any cause 12 months
Secondary Quality of life measured using Seattle Angina Questionnaire Quality of life measured using Seattle Angina Questionnaire at 24 hours post procedure, 1 month, 6 months and 12 months 12 months
Secondary Quality of life measured using EuroQoL-5D-5L questionnaire Quality of life measured using the EuroQoL-5D-5L questionnaire at 24 hours post procedure, 1 month, 6 months and 12 months 12 months
Secondary BARC 3-5 bleeding Incidence of Bleeding Academic Research Consortium (BARC) 3-5 classified bleeding as in-patient, and up to 12 months 12 months
Secondary Stroke Incidence of stroke 12 months
Secondary Cost effectiveness Cost effectiveness of immediate PCI versus standard care 12 months
Secondary Left ventricular ejection fraction on cardiac MRI Left ventricular ejection fraction on cardiac MRI 7 days (+/-3 days)
Secondary Infarct size on cardiac MRI Infarct size on cardiac MRI 7 days (+/-3 days)
Secondary Proportion of patients needing emergency/urgent revascularisation Proportion of patients needing emergency/urgent revascularisation (in group B) 3-4 days (standard of care timing angiography will vary between recruiting centres)
Secondary Total access site complications Incidence of total VARC-2 classified access site complications as in-patient, and up to 12 months 12 months
Secondary Major access site complications Incidence of major VARC-2 classified access site complications as in-patient, and up to 12 months 12 months
Secondary Sensitivity and specificity of novel biomarkers for predicting need for revascularisation Sensitivity and specificity of novel biomarkers in predicting which patients do or do not require PCI following diagnostic angiography 3-4 days (standard of care timing angiography will vary between recruiting centres)
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