Early Rheumatoid Arthritis COR Intervention

Not Applicable

Recruiting

• Conditions: Rheumatoid Arthritis; Cardiovascular Diseases
• Interventions: Other: Simvastatin; Other: Losartan; Other: Metformin; Other: Outpatient rheumatology department; Other: Refered to general practice

• Registration Number: NCT02246257
• Lead Sponsor: MD, PhD, Annemarie Lyng Svensson

Brief Summary

The primary aim of our present study is to evaluate the effect of a targeted, intensified, multidimensional intervention compared to conventional treatment of modifiable risk factors for CVD in patients with early RA. The primary endpoint, a composite of death from cardiovascular causes, non-fatal MI, non-fatal stroke and re-vascularisation, will be assessed after 5years' follow-up.

Detailed Description

The study is a prospective randomised open, blinded endpoint trial with balanced randomisation (1:1) conducted in seven outpatient clinics in Denmark. Follow-up visits for patients in the intervention group are scheduled to occur at baseline and then after 2, 4 and 12 weeks and thereafter every third month for 5 years after randomisation. The control group will be monitored for RA disease activity and comorbidity after 2, 4 weeks, 12 weeks and thereafter following national guidelines for RA. Prevention of CVD risk factors in the control group will be treated in general practice according to national guidelines for diabetes (2011), hypertension (2009) and CVD (2013).

Study Timeline

• Study Start: 2014-09
• Study First Submitted: 2014-09-17
• Study First Submitted QC: 2014-09-18
• Study First Posted: 2014-09-22
• Status Verified: 2022-05
• Last Update Submitted: 2022-05-20
• Last Update Posted: 2022-05-23
• Primary Completion: 2024-09
• Study Completion: 2024-09

Recruitment & Eligibility

• Status: RECRUITING
• Sex: All
• Target Recruitment: 300

Inclusion Criteria

• RA according to the revised American College of Rheumatology (ACR) 2010 criteria and plasma LDL > 2.5mmol/l.

Exclusion Criteria

• Pregnancy
• Lactation
• Ongoing/previous DMARD therapy
• Ongoing/previous steorid therapy
• Contraindication to any of the trial drugs
• Current infection with parvovirus B19, hepatitis B, hepatitis C or human immune deficiency virus. Previous report of hospitalisation for myocardial ischaemia defined as follows: a) non-fatal myocardial infarction (MI) defined according to national and international guidelines. b) Acute coronary syndrome (ACS) including acute ischaemic symptoms with possible biomarker changes or elctrocardiographic changes that to not meet the criteria for MI, c) angina pectoris, d) revascularisation (percutaneous coronary intervention (PCI) or coronary artery bypass grafting (CABG).

Study & Design

• Study Type: INTERVENTIONAL
• Study Design: PARALLEL

Arm && Interventions

Group	Intervention	Description
Intervention	Losartan	In the intervention group all patients will receive statins according to national guidelines. Stepwise introduction of pharmacological therapy targeting 1) hyperlipidaemia, 2) hypertension, 3) hyperglycaemia and 4) microalbuminuria and behaviour modification will be controlled by the project team in an outpatient rheumatology department. Hyperlipidaemia: LDL \> 2.5 is treated with 40 mg Simvastatin; Hypertension: BT \> 140/90 mmHg treated with 100 mg OD Losartan; Diabetes: DM BT \> 130/80 mmHg treated with 100 mg OD Losartan; Microalbuminuria: Urinary albumin creatinin ratio \> 30 mg treated with 100 mg OD Losartan; Hyperglycaemia: HBA1C \> 48 mmol/mol treated with 500 mg increased dose to 2,000 mg in 4 weeks Metformin
Control	Losartan	In the control group patients will be refered to general practice for pharmacological therapy according to national guidelines targeting 1) hyperlipidaemia, 2) hypertension, 3) hyperglycaemia and 4) microalbuminuria. Hyperlipidaemia: LDL \> 2.5 is treated with 40 mg Simvastatin; Hypertension: BT \> 140/90 mmHg treated with 100 mg OD Losartan; Diabetes: DM BT \> 130/80 mmHg treated with 100 mg OD Losartan; Microalbuminuria: Urinary albumin creatinin ratio \> 30 mg treated with 100 mg OD Losartan; Hyperglycaemia: HBA1C \> 48 mmol/mol treated with 500 mg increased dose to 2,000 mg in 4 weeks Metformin
Intervention	Metformin	In the intervention group all patients will receive statins according to national guidelines. Stepwise introduction of pharmacological therapy targeting 1) hyperlipidaemia, 2) hypertension, 3) hyperglycaemia and 4) microalbuminuria and behaviour modification will be controlled by the project team in an outpatient rheumatology department. Hyperlipidaemia: LDL \> 2.5 is treated with 40 mg Simvastatin; Hypertension: BT \> 140/90 mmHg treated with 100 mg OD Losartan; Diabetes: DM BT \> 130/80 mmHg treated with 100 mg OD Losartan; Microalbuminuria: Urinary albumin creatinin ratio \> 30 mg treated with 100 mg OD Losartan; Hyperglycaemia: HBA1C \> 48 mmol/mol treated with 500 mg increased dose to 2,000 mg in 4 weeks Metformin
Control	Simvastatin	In the control group patients will be refered to general practice for pharmacological therapy according to national guidelines targeting 1) hyperlipidaemia, 2) hypertension, 3) hyperglycaemia and 4) microalbuminuria. Hyperlipidaemia: LDL \> 2.5 is treated with 40 mg Simvastatin; Hypertension: BT \> 140/90 mmHg treated with 100 mg OD Losartan; Diabetes: DM BT \> 130/80 mmHg treated with 100 mg OD Losartan; Microalbuminuria: Urinary albumin creatinin ratio \> 30 mg treated with 100 mg OD Losartan; Hyperglycaemia: HBA1C \> 48 mmol/mol treated with 500 mg increased dose to 2,000 mg in 4 weeks Metformin
Intervention	Outpatient rheumatology department	In the intervention group all patients will receive statins according to national guidelines. Stepwise introduction of pharmacological therapy targeting 1) hyperlipidaemia, 2) hypertension, 3) hyperglycaemia and 4) microalbuminuria and behaviour modification will be controlled by the project team in an outpatient rheumatology department. Hyperlipidaemia: LDL \> 2.5 is treated with 40 mg Simvastatin; Hypertension: BT \> 140/90 mmHg treated with 100 mg OD Losartan; Diabetes: DM BT \> 130/80 mmHg treated with 100 mg OD Losartan; Microalbuminuria: Urinary albumin creatinin ratio \> 30 mg treated with 100 mg OD Losartan; Hyperglycaemia: HBA1C \> 48 mmol/mol treated with 500 mg increased dose to 2,000 mg in 4 weeks Metformin
Control	Refered to general practice	In the control group patients will be refered to general practice for pharmacological therapy according to national guidelines targeting 1) hyperlipidaemia, 2) hypertension, 3) hyperglycaemia and 4) microalbuminuria. Hyperlipidaemia: LDL \> 2.5 is treated with 40 mg Simvastatin; Hypertension: BT \> 140/90 mmHg treated with 100 mg OD Losartan; Diabetes: DM BT \> 130/80 mmHg treated with 100 mg OD Losartan; Microalbuminuria: Urinary albumin creatinin ratio \> 30 mg treated with 100 mg OD Losartan; Hyperglycaemia: HBA1C \> 48 mmol/mol treated with 500 mg increased dose to 2,000 mg in 4 weeks Metformin
Intervention	Simvastatin	In the intervention group all patients will receive statins according to national guidelines. Stepwise introduction of pharmacological therapy targeting 1) hyperlipidaemia, 2) hypertension, 3) hyperglycaemia and 4) microalbuminuria and behaviour modification will be controlled by the project team in an outpatient rheumatology department. Hyperlipidaemia: LDL \> 2.5 is treated with 40 mg Simvastatin; Hypertension: BT \> 140/90 mmHg treated with 100 mg OD Losartan; Diabetes: DM BT \> 130/80 mmHg treated with 100 mg OD Losartan; Microalbuminuria: Urinary albumin creatinin ratio \> 30 mg treated with 100 mg OD Losartan; Hyperglycaemia: HBA1C \> 48 mmol/mol treated with 500 mg increased dose to 2,000 mg in 4 weeks Metformin
Control	Metformin	In the control group patients will be refered to general practice for pharmacological therapy according to national guidelines targeting 1) hyperlipidaemia, 2) hypertension, 3) hyperglycaemia and 4) microalbuminuria. Hyperlipidaemia: LDL \> 2.5 is treated with 40 mg Simvastatin; Hypertension: BT \> 140/90 mmHg treated with 100 mg OD Losartan; Diabetes: DM BT \> 130/80 mmHg treated with 100 mg OD Losartan; Microalbuminuria: Urinary albumin creatinin ratio \> 30 mg treated with 100 mg OD Losartan; Hyperglycaemia: HBA1C \> 48 mmol/mol treated with 500 mg increased dose to 2,000 mg in 4 weeks Metformin

Primary Outcome Measures

Name	Time	Method
Time to Major Cardiac Event (death from cardiovascular causes, non-fatal myocardial infarction, non-fatal stroke and cardiac revascularization)	Up to 5 years	Days from randomization to the first of cardiac event. If no event, censoring occurs at earliest of termination date or efficacy cut-off date of 31 December 2020. Events will be adjudicated by an endpoint committee. Kaplan-Meier estimate of the mean.

Secondary Outcome Measures

Name	Time	Method
Time to Serious Adverse Event (hospitalizations)	Up to 5 years	Time from randomization to the first venous thromboembolic event. Kaplan-Meier estimate of the mean
Time to Death Due to Any Cause	Up to 5 years	Days from randomization to death. If no death then censoring occurs at earliest of termination date or efficacy cutoff date of 31 Dec 2020. Kaplan-Meier estimate of the mean
The proportion of patients having a treatment success	1, 2 and 5 years	* LDL cholesterol \< 2.5 mmol/l; * HbA1c \< 48 mmol/mol (HbA1c \< 6.5%),; * Blood pressure \< 140/90 mmHg for non-diabetic patients and \< 130/80 mm Hg for diabetic patients and normoalbuminuria (urinary albumin creatinine ratio \< 30 mg/g) after 1-year of follow-up this in agreement with present national guidelines, which will be adjusted accordingly to any future changes in the respective national guidelines.; * Low RA disease activity DAS28-CRP \< 3.2 and DAS28-CRP \< 2.6 at 12, 24 and 60 months. Furthermore, all to hospitalisations will be adjudicated by the event committee
Time to Non-cardiovascular Death	Up to 5 years	Days from randomization to death from a non-cardiovascular cause. If no event, then censoring occurs at earliest of termination date or efficacy cutoff date of 31 Dec 2020. Events will be adjudicated by an endpoint committee. Kaplan-Meier estimate of the mean

Trial Locations

Locations (1)

Department of Rheumathology, Frederiksberg and Bispebjerg univeristy Hospital; 🇩🇰 Frederiksberg, Region Of Copenhagen, Denmark