- ICH GCP
- US Clinical Trials Registry
- Clinical Trial NCT03796156
Aspirin to Target Arterial Events in Chronic Kidney Disease (ATTACK)
This study aims to find out whether people with chronic kidney disease [CKD] should take low dose aspirin to reduce the risk of first heart attack or stroke (cardiovascular disease [CVD]). CKD is common and is associated with an increased risk of CVD.
CVD is caused by small blood clots and aspirin thins the blood to reduce the risk of such clots developing but it also increases the risk of bleeding.
Aspirin is recommended to prevent further CVD in people who have already had a first CVD event (so called secondary prevention). Here the investigators want to study the use of aspirin as primary prevention in people with CKD who have not had a CVD to prevent the first event, to assess whether the potential benefits exceed the risks.
Eligible patients will be recruited from their United Kingdom (UK) general practices and allocated by chance to be prescribed once daily low dose aspirin or usual care only. Follow-up will be for several years both electronically (for general practice, hospital and mortality data) and by annual questionnaires to ascertain CVD and bleeding events.
Study Overview
Status
Intervention / Treatment
Detailed Description
Aim To test the hypothesis that the addition of 75mg aspirin once daily to usual care reduces the risk of major vascular events in patients with chronic kidney disease (CKD) who do not have pre-existing cardiovascular disease (CVD)
Design Open label, multi-centre randomised controlled trial
Setting UK general practices
Sample size 25,210 patients (12,605 per arm). A total of 1,827 major vascular events overall are required.
Eligibility Inclusion Criteria
- Males and females aged 18 years and over at the date of screening
- Subjects with CKD (reduced eGFR and/or albuminuria) defined as: • estimated glomerular filtration rate [eGFR] <60mL/min/1.73m2 for at least 90 days, and/or • kidney disease code on the GP electronic patient AND most recent eGFR in CKD-defining range (<60mL/min/1.73m2), and/or • albuminuria or proteinuria (defined as urine albumin:creatinine ratio [ACR] ≥3mg/mmol, and/or urine protein:creatinine ratio [PCR] ≥15mg/mmol, and/or +protein or greater on reagent strip)
- Subjects who are willing to give permission for their paper and electronic medical records to be accessed by trial investigators
- Subjects who are willing to be contacted and interviewed by trial investigators
- Subjects who can communicate well with the investigator or designee, understand the requirements of the study and understand and sign the written informed consent
Exclusion Criteria
- Subjects with CKD eGFR category 5
- Subjects with pre-existing cardiovascular disease (angina, myocardial infarction, stroke, transient ischaemic attack (TIA), significant peripheral vascular disease, coronary or peripheral revascularisation for atherosclerotic disease)
- Subjects with a current pre-existing condition associated with increased risk of bleeding other than CKD
- Subjects currently prescribed anticoagulants or antiplatelet agent, or taking over the counter (OTC) aspirin continuously
- Subjects who are currently and regularly taking other drugs with a potentially serious interaction with aspirin
- Subjects with a known allergy to aspirin or definite previous clinically important adverse reaction
- Subjects with poorly controlled hypertension (systolic blood pressure [BP] ≥180 mmHg and/or diastolic BP ≥105 mmHg)
- Subjects with other conditions which in the opinion of their General Practitioner (GP) would preclude prescription of aspirin in routine clinical practice, for example significant anaemia or thrombocytopenia.
- Subjects who are pregnant or likely to become pregnant during the study period
- Subjects with malignancy that is life-threatening or likely to limit prognosis, other life-threatening co-morbidity, or terminal illness
- Subjects whose behaviour or lifestyle would render them less likely to comply with study medication
- Subjects in prison
- Subjects currently participating in another clinical trial of an investigational medicinal product or who have taken part in such a trial in the last three months (Covid-19 vaccine studies are acceptable)
Interventions Suitable participants will be randomised to receive: 75mg non-enteric coated or dispersible aspirin once daily in addition to their usual medication; or no additional treatment and avoidance of aspirin.
Duration The trial will continue until at least 1,827 adjudicated primary endpoint events (major vascular events) have occurred, or before if the trial is discontinued after the internal pilot or for any other reason. It is anticipated that at least 6 years of recruitment (taking account a recruitment pause for the Covid-19 pandemic) and 2.5 years of follow-up will be required to complete the trial.
Randomisation and blinding Eligible participants, based on results of routine blood and urine tests at screening, will be randomised (open label randomisation) 1:1 to general practitioner (GP) prescription of aspirin vs. no prescription, stratified by age, diabetes and CKD severity.
Follow-up Data on potential CVD and bleeding outcomes will be collected electronically from GP records and national hospitalisation and mortality records. Adjudication panels (for CVD and for bleeding) will asses the information blind to allocation.
Patients will complete an annual quality of life questionnaire (EQ5D).
Outcomes. Primary outcome measure
Time to first major vascular event from the date of randomisation. A major vascular event is defined as a primary composite outcome of non-fatal myocardial infarction (MI), non-fatal stroke and cardiovascular death (excluding confirmed intracranial haemorrhage and other fatal cardiovascular haemorrhage).
Secondary outcome measures (all time to event except quality of life)
Efficacy
- Death from any cause
- Composite outcome of major vascular event or revascularisation (coronary and non-coronary)
- Individual components of the primary composite endpoint
- Health-related quality of life
Safety
- Composite outcome of intracranial haemorrhage (fatal and non-fatal), fatal extracranial haemorrhage and non-fatal major extracranial haemorrhage (adjudicated)
- Fatal and non-fatal (reported individually and as a composite) intracranial haemorrhage comprising: i) primary haemorrhagic stroke (to distinguish from haemorrhagic transformation of ischaemic stroke); ii) other intracranial haemorrhage (adjudicated). Intra-cranial haemorrhage will be sub-categorised as traumatic or non-traumatic.
- Fatal and non-fatal (reported individually and as a composite) major extracranial haemorrhage: i) upper gastrointestinal; ii) lower gastrointestinal; iii) sight-threatening ocular; iv) multiple trauma; v) other (adjudicated).
- Clinically relevant non-major bleeding if hospitalised (adjudicated).
- Composite outcome of fatal and non-fatal major extracranial haemorrhage and clinically relevant non-major bleeding (if hospitalised).
Tertiary (exploratory) outcome measures (all time to event except hospitalisation)
- Transient ischaemic attack
- Unplanned hospitalisation
- Hospitalisation with heart failure
- New diagnosis of cancer (colorectal/other)
- Death due to cancer (where cancer is the underlying cause of death)
- CKD progression
- New diagnosis of dementia
- Major non-traumatic lower limb amputation
Statistical methods The primary outcome measure of time to first major vascular event will be analysed for the intention-to-treat (ITT) population. Deaths from other causes (including fatal bleeding) will be treated as competing events. Patients who do not experience a major vascular event will be censored at the date of last follow-up.
All primary, secondary and tertiary time to event outcomes will be described using Kaplan-Meier curves or Cumulative Hazard plots for time to event outcomes involving competing risks for the ITT population. Analyses of time to event outcomes will be performed using Cox proportional hazards models or Competing Risk regression models, both unadjusted and adjusted for stratification factors: age, diabetes and CKD severity.
The adjusted Competing Risk regression model for time to first major vascular event, with deaths from other causes (including fatal bleeding) treated as competing events, and patients who do not experience a major vascular event censored, will form the primary endpoint analysis model.
Other secondary and tertiary endpoints will be assessed by arm using summary statistics (e.g. Pearson's χ² tests) in the ITT population.
The amount of missing data and reasons for the incompleteness will be explored and presented overall i.e. not by group. If the amount of missing data is deemed too high and if appropriate (i.e. assuming the missing data is either missing at random [MAR] or missing completely at random [MCAR] and censoring assumed to be non-informative), multiple imputation will be performed accordingly, for which all covariates included in the multivariable model, together with the censoring/event indicator and the cumulative baseline hazard will be included in the multiple imputation model.
Health economic analysis will also be undertaken.
Study Type
Enrollment (Anticipated)
Phase
- Phase 3
Contacts and Locations
Study Contact
- Name: Jennifer Dumbleton
- Phone Number: 00441158231053
- Email: jennifer.dumbleton@nottingham.ac.uk
Study Contact Backup
- Name: Diane Stevenson
- Phone Number: 00441158231053
- Email: diane.stevenson@nottingham.ac.uk
Study Locations
-
-
-
Nottingham, United Kingdom, NG72UH
- Recruiting
- Nottingham Digestive Diseases Centre
-
Contact:
- Jennifer Dumbleton
- Phone Number: 00441158231053
- Email: jennifer.dumbleton@nottingham.ac.uk
-
Contact:
- Diane Stevenson
- Phone Number: 00441158231053
- Email: diane.stevenson@nottingham.ac.uk
-
-
Participation Criteria
Eligibility Criteria
Ages Eligible for Study
Accepts Healthy Volunteers
Description
Inclusion Criteria:
- Males and females aged 18 years and over at the date of screening
- .Subjects with CKD (reduced eGFR and/or albuminuria) defined as: • estimated glomerular filtration rate [eGFR] <60mL/min/1.73m2 for at least 90 days, and/or • kidney disease code on the GP electronic patient AND most recent eGFR in CKD-defining range (<60mL/min/1.73m2), and/or • albuminuria or proteinuria (defined as urine albumin:creatinine ratio [ACR] ≥3mg/mmol, and/or urine protein:creatinine ratio [PCR] ≥15mg/mmol, and/or +protein or greater on reagent strip)
- Subjects who are willing to give permission for their paper and electronic medical records to be accessed by trial investigators
- Subjects who are willing to be contacted and interviewed by trial investigators
- Subjects who can communicate well with the investigator or designee, understand the requirements of the study and understand and sign the written informed consent
Exclusion Criteria
- Subjects with CKD GFR category 5
- Subjects with pre-existing cardiovascular disease (angina, myocardial infarction, stroke, transient ischaemic attack (TIA), significant peripheral vascular disease, coronary or peripheral revascularisation for atherosclerotic disease)
- Subjects with a current pre-existing condition associated with increased risk of bleeding other than CKD
- Subjects currently prescribed anticoagulants or antiplatelet agent, or taking over the counter (OTC) aspirin continuously
- Subjects who are currently and regularly taking other drugs with a potentially serious interaction with aspirin
- Subjects with a known allergy to aspirin or definite previous clinically important adverse reaction
- Subjects with poorly controlled hypertension (systolic blood pressure [BP] ≥180 mmHg and/or diastolic BP ≥105 mmHg)
- . Subjects with other conditions which in the opinion of their General Practitioner (GP) would preclude prescription of aspirin in routine clinical practice, for example significant anaemia or thrombocytopenia
- Subjects who are pregnant or likely to become pregnant during the study period
- Subjects with malignancy that is life-threatening or likely to limit prognosis, other life-threatening co-morbidity, or terminal illness
- Subjects whose behaviour or lifestyle would render them less likely to comply with study medication
- Subjects in prison
- Subjects currently participating in another clinical trial of an investigational medicinal product or who have taken part in such a trial in the last three months (Covid-19 vaccine studies are acceptable)
Study Plan
How is the study designed?
Design Details
- Primary Purpose: Prevention
- Allocation: Randomized
- Interventional Model: Parallel Assignment
- Masking: Single
Arms and Interventions
Participant Group / Arm |
Intervention / Treatment |
---|---|
Experimental: Aspirin
75mg of non enteric coated or dispersible aspirin once daily added to usual medications
|
75mg low dose non enteric coated or dispersible
|
No Intervention: Usual care
Usual medications only
|
What is the study measuring?
Primary Outcome Measures
Outcome Measure |
Measure Description |
Time Frame |
---|---|---|
Number of participants with a Major vascular event: Composite outcome of non-fatal myocardial infarction, non-fatal stroke and cardiovascular death (excluding confirmed intracranial haemorrhage and other fatal cardiovascular haemorrhage)
Time Frame: Over average 4 years follow-up
|
Acute MI defined according to the Third Universal Definition of myocardial infarction (MI). Acute stroke defined in accordance with the World Health Organization (WHO) definition as "rapidly developing clinical signs of focal (or global) disturbance of cerebral function, with symptoms lasting 24 hours or longer, with no apparent cause other than of vascular origin". This excludes cases of primary cerebral tumour, cerebral metastasis, subdural haematoma, post-seizure palsy, brain trauma and TIA. Haemorrhagic stroke (fatal and non-fatal) including intracerebral haemorrhage and SAH which has been confirmed on appropriate imaging is excluded from the primary composite endpoint and included within the secondary endpoints. |
Over average 4 years follow-up
|
Secondary Outcome Measures
Outcome Measure |
Measure Description |
Time Frame |
---|---|---|
Number of participants dying from any cause
Time Frame: Average 4 years follow-up
|
Death from any cause
|
Average 4 years follow-up
|
Number of participants with major vascular events plus revascularisation
Time Frame: Average 4 years follow-up
|
Primary outcome plus coronary and non coronary arterial revascularisation.
It will include open and percutaneous coronary and non-coronary (including carotid, aortic and limb) procedures (as defined in Office of Population Censuses and Surveys OPCS-4 procedure codes) and will be ascertained from Hospital Episode Statistics (HES) data.
|
Average 4 years follow-up
|
Number of participants with Non-fatal myocardial infarction
Time Frame: Average 4 years follow-up
|
Non-fatal myocardial infarction.
Acute MI defined according to the Third Universal Definition of myocardial infarction (MI).
|
Average 4 years follow-up
|
Health-related quality of life, mean utility score
Time Frame: Average 4 years follow-up
|
Euroqol EQ-5D utility score derived from 5 states (scoring 1-5) converted to utility values using UK general population set
|
Average 4 years follow-up
|
Number of participants with intra-cranial haemorrhage, fatal and non fatal major extra cranial haemorrhage
Time Frame: Average 4 years follow-up
|
Intra-cranial haemorrhage includes intracerebral haemorrhage, subarachnoid haemorrhage, subdural haemorrhage, and extradural haemorrhage. Extra-cranial haemorrhage is:
In particular, to be classified as major, bleeds in a critical area or organ should:
|
Average 4 years follow-up
|
Number of participants with Fatal and non-fatal intra-cranial haemorrhage
Time Frame: Average 4 years follow-up
|
Fatal and non-fatal intra-cranial haemorrhage as above It comprises primary haemorrhagic stroke(to distinguish from haemorrhagic transformation of ischaemic stroke) ii)other intra-cranial haemorrhage (adjudicated).
Intra-cranial haemorrhage will be sub categorised as traumatic and non-traumatic.
|
Average 4 years follow-up
|
Number of participants with Fatal and non-fatal major extra-cranial haemorrhage
Time Frame: Average 4 years follow-up
|
Fatal and non-fatal major extra-cranial haemorrhage as above.
Categorised as i) upper-gastro-intestinal ii) lower gastro-intestinal iii) sight threatening ocular iv)multiple trauma v) other
|
Average 4 years follow-up
|
Number of participants with Clinically relevant non major bleeding (hospitalised)
Time Frame: Average 4 years follow-up
|
Defined in accordance with the International Society on Thrombosis and Haemostasis (ISTH) as any sign or symptom of haemorrhage (e.g. more bleeding than would be expected for a clinical circumstance, including bleeding found by imaging alone) that does not fit the criteria for the ISTH definition of major bleeding but does meet at least one of the following criteria: • Leading to hospitalisation This definition excludes all minor bleeding episodes that lead to medical evaluation involving direct patient contact. |
Average 4 years follow-up
|
Number of participants with Non-fatal stroke
Time Frame: Average 4 years follow-up
|
Non-fatal stroke excluding confirmed intracranial haemorrhage.
Acute stroke defined in accordance with the World Health Organization (WHO) definition as "rapidly developing clinical signs of focal (or global) disturbance of cerebral function, with symptoms lasting 24 hours or longer, with no apparent cause other than of vascular origin".
This excludes cases of primary cerebral tumour, cerebral metastasis, subdural haematoma, post-seizure palsy, brain trauma and TIA.
Haemorrhagic stroke ( including intracerebral haemorrhage and sub-arachnoid haemorrhage) which has been confirmed on appropriate imaging is excluded.
|
Average 4 years follow-up
|
Number of participants with Cardiovascular death
Time Frame: Average 4 years follow-up
|
Cardiovascular death (excluding confirmed intracranial haemorrhage and other fatal cardiovascular haemorrhage).
|
Average 4 years follow-up
|
Number of participants with fatal and non fatal major extra-cranial haemorrhage and clinically relevant non major bleed (if hospitalised)
Time Frame: Average 4 years follow-up
|
Definitions above
|
Average 4 years follow-up
|
Other Outcome Measures
Outcome Measure |
Measure Description |
Time Frame |
---|---|---|
Number of participants with transient ischaemic attack
Time Frame: Average 4 years follow-up
|
A transient episode of neurological dysfunction caused by focal brain spinal cord or retinal ischemia without acute infarction
|
Average 4 years follow-up
|
Number of Unplanned hospitalisations per participant
Time Frame: Average 4 years follow-up
|
Defined as an official admission that is for a duration greater than 24 hours or a minimum of 2 calendar days where exact time of stay is unavailable.
|
Average 4 years follow-up
|
Number of participants with new diagnosis of cancer
Time Frame: Average 4 years follow-up
|
Any new cancer diagnosis excluding non melanotic skin cancer
|
Average 4 years follow-up
|
Number of participants with CKD progression
Time Frame: Average 4 years follow-up
|
Defined as at least one of:
|
Average 4 years follow-up
|
Number of participants with new diagnosis of dementia
Time Frame: Average 4 years follow-up
|
Coded dementia (ICD, Read) from linked GP and hospital data
|
Average 4 years follow-up
|
Hospitalisation with heart failure
Time Frame: Average 4 years follow-up
|
Coded heart failure (ICD) from hospitalisation data
|
Average 4 years follow-up
|
Death due to cancer (where cancer is the underlying cause of death)
Time Frame: Average 4 years follow-up
|
Average 4 years follow-up
|
|
Major non traumatic lower limb amputation
Time Frame: Average 4 years follow-up
|
Below or above knee amputation, coded (ICD) from hospitalisation data
|
Average 4 years follow-up
|
Collaborators and Investigators
Sponsor
Collaborators
Investigators
- Principal Investigator: Hugh Gallagher, MD, Epsom and St Helier University Hospitals NHS Trust
- Principal Investigator: Paul Roderick, MD, University of Southampton
Publications and helpful links
General Publications
- Natale P, Palmer SC, Saglimbene VM, Ruospo M, Razavian M, Craig JC, Jardine MJ, Webster AC, Strippoli GF. Antiplatelet agents for chronic kidney disease. Cochrane Database Syst Rev. 2022 Feb 28;2(2):CD008834. doi: 10.1002/14651858.CD008834.pub4.
- Gallagher H, Dumbleton J, Maishman T, Whitehead A, Moore MV, Fuat A, Fitzmaurice D, Henderson RA, Lord J, Griffith KE, Stevens P, Taal MW, Stevenson D, Fraser SD, Lown M, Hawkey CJ, Roderick PJ. Aspirin to target arterial events in chronic kidney disease (ATTACK): study protocol for a multicentre, prospective, randomised, open-label, blinded endpoint, parallel group trial of low-dose aspirin vs. standard care for the primary prevention of cardiovascular disease in people with chronic kidney disease. Trials. 2022 Apr 21;23(1):331. doi: 10.1186/s13063-022-06132-z.
Study record dates
Study Major Dates
Study Start (Actual)
Primary Completion (Anticipated)
Study Completion (Anticipated)
Study Registration Dates
First Submitted
First Submitted That Met QC Criteria
First Posted (Actual)
Study Record Updates
Last Update Posted (Actual)
Last Update Submitted That Met QC Criteria
Last Verified
More Information
Terms related to this study
Additional Relevant MeSH Terms
- Pathologic Processes
- Urologic Diseases
- Disease Attributes
- Renal Insufficiency
- Chronic Disease
- Female Urogenital Diseases
- Female Urogenital Diseases and Pregnancy Complications
- Urogenital Diseases
- Male Urogenital Diseases
- Cardiovascular Diseases
- Kidney Diseases
- Renal Insufficiency, Chronic
- Physiological Effects of Drugs
- Molecular Mechanisms of Pharmacological Action
- Peripheral Nervous System Agents
- Enzyme Inhibitors
- Analgesics
- Sensory System Agents
- Anti-Inflammatory Agents, Non-Steroidal
- Analgesics, Non-Narcotic
- Anti-Inflammatory Agents
- Antirheumatic Agents
- Fibrinolytic Agents
- Fibrin Modulating Agents
- Platelet Aggregation Inhibitors
- Cyclooxygenase Inhibitors
- Antipyretics
- Aspirin
Other Study ID Numbers
- 31844
Plan for Individual participant data (IPD)
Plan to Share Individual Participant Data (IPD)?
Drug and device information, study documents
Studies a U.S. FDA-regulated drug product
Studies a U.S. FDA-regulated device product
This information was retrieved directly from the website clinicaltrials.gov without any changes. If you have any requests to change, remove or update your study details, please contact register@clinicaltrials.gov. As soon as a change is implemented on clinicaltrials.gov, this will be updated automatically on our website as well.
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