Increased Risk of Major Cardiovascular Events in a Nationwide Cohort of Rheumatoid Arthritis Patients Treated with Biological Agents

Signe Abitz Winther¹, Peter Riis Hansen¹, Søren Lund Kristensen¹, Lene Dreyer², Ole Ahlehoff¹, Louise Linde³, Christian Torp-Pedersen¹ and Jesper Lindhardsen¹, ¹Department of Cardiology, Copenhagen University Hospital Gentofte, Hellerup, Denmark, ²Internal Medicine - Rheumatology Section, Copenhagen University Hospital at Gentofte, Copenhagen, Denmark, ³Internal Medicine - Rheumatology Section, Copenhagen University Hospital Gentofte, Hellerup, Denmark

Meeting: 2012 ACR/ARHP Annual Meeting

Keywords: biologic response modifiers, cardiovascular disease and rheumatoid arthritis, treatment

Session Information

Title: Rheumatoid Arthritis - Clinical Aspects III: Rheumatoid Arthritis and Cardiovascular Disease

Session Type: Abstract Submissions (ACR)

Background/Purpose:

Patients with rheumatoid arthritis (RA) are at increased risk of cardiovascular disease, but in contrast to the well-established risk of myocardial infarction (MI), the results from studies on RA-related risk of stroke have been inconsistent. Also, we recently found an association between RA and atrial fibrillation (AF), which is an important risk factor for stroke. Most of these data, however, stem from more dated cohorts where the RA-specific treatment was less aggressive than today. Consequently, this study examined the incidence of MI, stroke and AF in a large, unselected, nationwide cohort of biologically treated RA patients.

Methods:

In Denmark, biological RA treatment is provided at no cost, but patients are required to be registered and followed in the DANBIO registry. All RA patients treated with biological agents during the period 2001-2009 were matched with 10 individuals from the general population by age and sex at the start of biological therapy. Through individual-level linkage to the National Patient Register, the National Register of Medicinal Products (national prescription database) and the National Civil Register, participants were characterized with respect to comorbidity, pharmacotherapy and socioeconomic status and subsequently monitored for the outcomes of interest (MI, stroke, or AF) until emigration, death, or December 31, 2010. Incidence rates were calculated and multivariable proportional hazard models were fitted to estimate risk of outcomes in terms of hazard ratios.

Results:

A total of 3872 RA patients and 38720 controls were included. Cohort participants were predominantly women (74%) and had a mean age of 56 years. Cardiovascular and RA-specific characteristics are listed in Table 1. The cohort was followed for a mean of 4.5 years during which 639 MIs, 867 strokes and 804 cases of AF occurred. The risk of all outcomes was significantly increased in biologically treated RA patients with a 95% excess risk of MI, 31% excess risk of stroke, and 35% excess risk of AF in the fully adjusted analysis (Table 2).

Conclusion:

In a large, nationwide and well-characterized cohort of RA patients treated with biological agents, the risk of MI was approximately two times higher than in the general population, while the excess risk of stroke and AF was less pronounced. The results indicate that despite aggressive treatment of RA the risk of major cardiovascular events is increased in these patients.

Table 1: Baseline characteristics

	Biologically treated RA patients n=3872	Controls n=38720
Age	56 (±13) years	56 (±13) years
Females	2861 (74 %)	28610 (74 %)
Follow-up	4.5 years	4.5 years
Pharmacological treatment
Aspirin	403 (10.4 %)	3604 (9.3 %)
Beta blockers	462 (11.9 %)	3574 (9.2 %)
RAS inhibitors	554 (14.3 %)	5057 (13.1 %)
Lipid-lowering drugs	333 (8.6 %)	3917 (10.1 %)
NSAIDs	2710 (70.0 %)	8691 (22.4 %)
DMARDs	2944 (76.0 %)	0 (0.0%)
Charlson co-morbidity index	0.06 (±0.36)	0.06 (±0.39)
Previous CV disease
Myocardial infarction	107 (2.8 %)	704 (1.8 %)
Stroke	68 (1.8 %)	795 (2.1 %)
Atrial fibrillation	103 (2.7 %)	777 (2.0 %)
Socioeconomic status (1=low to 4=high)	2.51 (1.04)	2.50 (1.13)
RA-specific characteristics
RA duration	8 (3-16) years	–
HAQ score	1.25 (0.73-1.75)	–
DAS28crp score	5.1 (4.1-5.9)	–
CRP	14 (7-32) mg/l	–
HAQ, Health Assessment Questionnaire; DAS, Disease activity score; RAS, Renin-angiotensin system; NSAID, Non-steroidal anti-inflammatory drug; DMARD, Disease-modifying anti-rheumatic drug; CV, cardiovascular; CRP, C-reactive protein. Numbers are means (±SD), n (%) and medians (interquartile range) as appropriate.

Table 2: Risk of adverse cardiovascular events in biologically treated RA patients versus controls (reference)

	Myocardial infarction		Stroke		Atrial Fibrillation
	RA	Controls	RA	Controls	RA	Controls
Events (n)	106	533	98	769	103	701
Incidence rate (events per 1000 py)	5.7	2.8	5.2	4.1	5.7	3.9
Risk models	Hazard ratios (95% CI)
Unadjusted	1.98 (1.60-2.44)		1.31 (1.06-1.62)		1.41 (1.14-1.73)
As above + co-morbidity and socioeconomic status	2.02 (1.63-2.49)		1.33 (1.08-1.65)		1.42 (1.15-1.75)
As above + CV medication and previous CV disease*	1.95 (1.57-2.43)		1.31 (1.05-1.63)		1.35 (1.09-1.68)
py, person-years; CI, confidence interval; CV, cardiovascular. * Covariates included individually (as outlined in Table 1).

Disclosure:

S. A. Winther,
None;

P. R. Hansen,
None;

S. L. Kristensen,
None;

L. Dreyer,
None;

O. Ahlehoff,
None;

L. Linde,
None;

C. Torp-Pedersen,
None;

J. Lindhardsen,
None.

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