C-reactive protein: the underlying cause of microvascular dysfunction in rheumatoid arthritis

doi:10.1093/rheumatology/ken386

Rheumatology Advance Access published online on October 14, 2008
Rheumatology, doi:10.1093/rheumatology/ken386

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C-reactive protein: the underlying cause of microvascular dysfunction in rheumatoid arthritis

B. Galarraga¹, F. Khan¹, P. Kumar¹, T. Pullar¹ and J. J. F. Belch¹

¹The Institute of Cardiovascular Research, Vascular and Inflammatory Diseases Research Unit, University Division of Medicine and Therapeutics, Ninewells Hospital and Medical School, Dundee, UK.

Correspondence to: B. Galarraga, The Institute of Cardiovascular Research, Vascular and Inflammatory Diseases Research Unit, University Division of Medicine and Therapeutics, Ninewells Hospital and Medical School, Dundee DD1 9SY, UK. E-mail: Lauberdoc{at}hotmail.com

Abstract

Objective. RA is a chronic autoimmune inflammatory conditionassociated with increased cardiovascular morbidity and mortality.Endothelial dysfunction, a marker of early atherosclerotic disease,occurs in some inflammatory diseases but this relationship hasnot been previously explored within the microvasculature ofpatients with RA. We therefore assessed forearm microvascularendothelial function in patients with RA and determined itsrelationship to RA disease activity and inflammation.

Methods. A total of 128 RA patients with no previous historyof cardiovascular disease were evaluated. Endothelium-dependentand -independent forearm skin microvascular function was measuredusing laser Doppler imaging after iontophoretic delivery ofacetylcholine (ACh) and sodium nitroprusside (SNP), respectively.Parameters of RA disease activity and inflammation were alsochecked.

Results. There was a significant negative correlation betweenthe level of inflammation measured by log₁₀CRP and maximum vasodilatationmeasured by peak ACh response (r² = –0.209, P = 0.018,Pearson correlation test). In a multiple regression model, age(β = –0.449, P < 0.0001) and log₁₀CRP (β= –0.193, P = 0.026) were independently negatively associatedwith ACh responses. When RA patients were sub-divided accordingto their systemic inflammatory status (CRP > 10 mg/l vs CRP $≤$ 10 mg/l), the high CRP group showed lower vasodilator responsesto ACh [P = 0.018, analysis of variance (ANOVA)] and SNP (P= 0.05, ANOVA) than the low CRP group.

Conclusions. In this large cross-sectional study, we found forthe first time systemic inflammation (CRP) to be independentlyassociated with microvascular dysfunction in patients with RA.This strong correlation was independent of other conventionalvascular risk factors.

KEY WORDS: Endothelium, Inflammation, Microcirculation, Rheumatoid arthritis, C-reactive protein, Cardiovascular disease

Submitted 16 June 2008; revised version accepted 4 September 2008.
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