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Clinical Trial Details — Status: Enrolling by invitation

Administrative data

NCT number NCT03674255
Other study ID # 18100
Secondary ID
Status Enrolling by invitation
Phase
First received
Last updated
Start date March 2015
Est. completion date January 2032

Study information

Verified date February 2020
Source University of Oxford
Contact n/a
Is FDA regulated No
Health authority
Study type Observational

Clinical Trial Summary

EVAREST will identify and validate novel blood and imaging biomarkers of potential value for consistent and accurate interpretation of stress echocardiography. During phase one, blood samples will be collected to assess the impact of cardiac stress on levels of circulating biomarkers and examine whether the measurement of these biomarkers can provide additional prognostic information. Phases one, two and three will also determine whether novel imaging biomarkers can be identified in the echocardiograms that can be used for objective interpretation of the stress echocardiograms. EVAREST will recruit up to 8000 patients (First 500 during phase one, an additional 500 during phase two and an additional 7000 during phase three) from multiple hospitals across United Kingdom, who have been referred for a stress echocardiogram as part of their investigations into ischaemic heart disease. Phase four of the study will continue into a clinical study cohort phase to capture information from all patients referred for a stress echocardiogram in the UK, regardless of the reason for investigation.This registry phase will run for 2 years, recruiting up to 15000 participants.


Description:

Study Overview:

• Design

EVAREST is a multi-centre observational study comparing accuracy of novel quantitative stress echocardiography biomarkers for prediction of 12 month outcome against standard clinical interpretation.

• Scientific Justification

Coronary artery disease affects 2.3 million people in the UK and is responsible for 66 000 deaths each (BHF, 2018). As such, early diagnosis and intervention is crucial for saving lives and improving people's quality of life. Stress echocardiography is a commonly used, non-invasive imaging test used for detection of prognostically significant coronary artery disease. It allows the detection of regional wall motion abnormalities (RWMAs) which develop when the myocardium is not receiving adequate perfusion and, as such, indicates obstructive coronary artery disease. Average sensitivity and specificity for stress echocardiography is estimated at 81% and 82%, respectively (Geleijnse et al., 2009) in meta-analysis but remains highly subjective (Hoffmann et al., 1996) and subject to operator skill (Picano et al., 1991). Objective, quantifiable biomarkers in blood samples, or from images, acquired during the stress echocardiogram, which predict outcome of patients, could be used to reduce variability of stress echocardiography and ensure consistent and accurate results.

Aims

- To establish whether the measurement of specific blood biomarkers, in particular, extracellular vesicles, during a stress echocardiogram, can give additional prognostic information to stress echocardiography.

- To establish whether imaging biomarkers can provide additional prognostic information to stress echocardiography.

Phase One

Phase one will investigate the impact of cardiac stress on the levels of circulating biomarkers, in particular, extracellular vesicles. This phase will also assess whether they provide further prognostic information in addition to the echocardiogram. Blood samples will be collected from a cannula (inserted for the standard clinical procedure) before stress, during peak stress and during recovery and analysed to determine whether there were any changes in circulating extracellular vesicles during these three stages and whether these differ between patients with and without ischaemic heart disease.

Phase Two

Phase two continues recruitment for collection of stress echocardiogram images. Data collected during this phase will be compared with the data obtained during phase one to assess the usefulness of incorporating blood biomarkers into assessment of stress echocardiograms. In addition, the images obtained during phase two will be combined with the images collected during phase one to allow for the identification of novel imaging biomarkers which can be used to assist in the identification of patients with prognostically significant coronary disease.

Phase Three

Phase three will expand recruitment to allow evaluation of the generalisability of the imaging biomarkers identified in phase one and two across different healthcare settings, operators, stress protocols, machines and patient groups.

Phase Four

The fourth phase of the study allows for an assessment of all stress echocardiography practise in the UK and the demographics of patients being referred for stress echocardiogram. Phase four will investigate the use of stress echocardiography as a clinical procedure in the UK.

• Recruitment, Consent and Data Collection

Patients who have been scheduled a stress echocardiogram (using either pharmacological or exercise stress) as part of clinical investigations will be sent a participant information leaflet to read prior to their clinic appointment. When they are in the department, they will be approached by a study investigator to see whether they would be interested in taking part in the study and have the opportunity to ask the investigator any questions so that they fully understand the study. If they are interested in taking part, the process of obtaining informed consent will take place.

Following consent, the images acquired during the stress echocardiogram will be downloaded and anonymised with the participant's unique study ID number. These images will be transferred to the Oxford Research Echocardiography Core Laboratory (ORECL) for further analysis. Relevant medical history will be obtained for each participant as well as the clinician's interpretation of the echocardiogram. One year after the initial stress echocardiogram (range: 11-18 months), the participant will be followed-up to determine whether they underwent any further investigations for ischaemic heart disease (such as coronary angiography, cardiac magnetic resonance imaging, myocardial perfusion scintigraphy or repeat stress echocardiography) or had any coronary events. The participant may also be contacted via telephone to find out whether they were admitted to any other hospital for investigations. For phase one participants only, three blood samples (totalling approximately 40 ml) will be obtained before, at peak stress and after a recovery period, for the assessment of blood biomarkers. These samples will be taken through the cannula inserted as is routine during stress echocardiography. Participants will also give consent for follow-up information to be accessed for up to ten years after their initial stress echocardiogram.

• Outcome Assessment

Patient outcomes will be examined by an adjudication committee, blinded to the results of the stress echocardiograms. This committee will be led by a cardiologist and will examine all information obtained for a participant after the follow-up period has concluded. The criteria for confirming the presence of significant coronary artery disease include > 70% stenosis (assessed either via invasive coronary angiography or CT coronary angiography), an FFR < 0.85 or disease requiring intervention (either by percutaneous coronary intervention (PCI) or coronary artery bypass grafts (CABG)). Other end-points include coronary events (such as myocardial infarction) or death (attributed to coronary artery disease). If a patient has had no further investigations or events since their stress echocardiogram, their outcome will be recorded as normal.

• Confidentiality

All data obtained will be securely stored in accordance with the General Data Protection Regulations and Data Protection Act (2018) and Caldicott Principles.


Recruitment information / eligibility

Status Enrolling by invitation
Enrollment 23000
Est. completion date January 2032
Est. primary completion date March 2020
Accepts healthy volunteers No
Gender All
Age group 18 Years and older
Eligibility Inclusion Criteria:

- Patients must be undergoing a stress echocardiogram to investigate the presence of ischaemic heart disease (groups 1-3).

- Patients must be able to provide informed consent.

- Patients must be aged over 18 years of age.

Exclusion Criteria:

- Patients undergoing stress echocardiography to assess valvular function.

- Patients who are unwilling or unable to provide informed consent.

- Patients aged under 18 years of age.

Study Design


Locations

Country Name City State
n/a

Sponsors (33)

Lead Sponsor Collaborator
University of Oxford Blackpool Teaching Hospitals NHS Foundation Trust, Bradford Teaching Hospitals NHS Foundation Trust, Buckinghamshire Healthcare NHS Trust, Calderdale and Huddersfield NHS Foundation Trust, Chelsea and Westminster Hospital NHS Foundation Trust, East Lancashire Hospitals NHS Trust, East Suffolk and North Essex NHS Foundation Trust, Great Western Hospital NHS Foundation Trust, Guy's and St Thomas' NHS Foundation Trust, Hampshire Hospitals NHS Foundation Trust, King's College Hospital NHS Trust, Lantheus Medical Imaging, London North West Healthcare NHS Trust, Mid Essex Hospital NHS Trust, Mid Yorkshire Hospitals NHS Trust, Milton Keynes University Hospital NHS Foundation Trust, National Institute for Health Research, United Kingdom, North Middlesex University Hospital, North West Anglia NHS Foundation Trust, Northampton General Hospital NHS Trust, Northumbria Healthcare NHS Foundation Trust, Nottingham University Hospitals NHS Trust, Oxford University Hospitals NHS Trust, Poole Hospital NHS Foundation Trust, Royal Berkshire NHS Foundation Trust, Royal United Hospital Bath NHS Trust, St George's University Hospitals NHS Foundation Trust, Tameside Hospital NHS Foundation Trust, Ultromics Ltd, University Hospitals Bristol NHS Foundation Trust, Wrightington, Wigan and Leigh NHS Foundation Trust, Yeovil District Hospital NHS Foundation Trust

References & Publications (3)

Alsharqi M, Upton R, Mumith A, Leeson P. Artificial intelligence: a new clinical support tool for stress echocardiography. Expert Rev Med Devices. 2018 Aug;15(8):513-515. doi: 10.1080/17434440.2018.1497482. Epub 2018 Jul 19. Review. — View Citation

Augustine D, Ayers LV, Lima E, Newton L, Lewandowski AJ, Davis EF, Ferry B, Leeson P. Dynamic release and clearance of circulating microparticles during cardiac stress. Circ Res. 2014 Jan 3;114(1):109-13. doi: 10.1161/CIRCRESAHA.114.301904. Epub 2013 Oct 18. — View Citation

Ayers L, Nieuwland R, Kohler M, Kraenkel N, Ferry B, Leeson P. Dynamic microvesicle release and clearance within the cardiovascular system: triggers and mechanisms. Clin Sci (Lond). 2015 Dec;129(11):915-31. doi: 10.1042/CS20140623. Review. — View Citation

Outcome

Type Measure Description Time frame Safety issue
Primary Assessment of Prognostically Significant CAD Patients will be followed up one year after their stress echocardiogram to determine whether they have prognostically significant CAD. This is defined as >70% stenosis assessed by angiography (either via invasive coronary angiography or CT coronary angiography), an FFR< 0.85 or the intention to revascularize (either via PCI or CABG). Any tests that occur in a ten year period after the stress echocardiogram will also be recorded. Data will be collected for ten years after the patient undergoes the stress echocardiogram.
Primary Examination of Medical Records Medical records will also be examined to check for any acute coronary syndromes within the year following the stress echocardiogram. Participants will also be contacted by telephone to capture any out-of-hospital events. Further follow-up data will be captured up to 10 years after the patient's initial stress echocardiogram. Data will be collected for ten years after the patient undergoes the stress echocardiogram.
Secondary Quantification of Extracellular Vesicles (obtained from blood samples) by Flow Cytometry The concentration of a comprehensive panel of cell-derived extracellular vesicles (such as erythrocyte, endothelial and platelet-derived extracellular vesicles) will be measured via flow cytometry in both the pre-stress and post-stress blood samples to assess the effect of cardiac stress on their concentration. The concentrations will also be compared between the patients with and without prognostically significant coronary artery disease to determine whether the concentration of extracellular vesicles is affected by coronary artery disease. Blood samples will be obtained before and after the stress echocardiogram. Analysis will be complete one year from the date of the stress echocardiogram
Secondary Assessment of Time to Diagnosis We will assess whether the use of novel imaging and blood biomarkers can reduce the time to diagnosis of prognostically significant CAD. Data will be collected for ten years after the patient undergoes the stress echocardiogram.
Secondary Analysis of Potential Cost Savings Through the Use of Novel Biomarkers By the Reduction in Unnecessary Procedures Health economic assessment will be carried out to determine whether the inclusion of imaging and blood biomarkers in the diagnostic process can ultimately lead to cost reductions through the reduction in unnecessary procedures and treatments. Data will be collected for ten years after the patient undergoes the stress echocardiogram.
Secondary Investigation into the use of stress echocardiography as a clinical procedure in the UK. Analysis of the number and type of stress echocardiograms performed across UK NHS sites as well as demographic information on the patients referred for stress echocardiography and accuracy of stress echocardiography, using follow-up data. Data will be collected for ten years after the patient undergoes the stress echocardiogram.
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