RT Journal Article SR Electronic T1 Cholesteryl Ester Transfer Protein in Patients with Rheumatoid Arthritis JF The Journal of Rheumatology JO J Rheumatol FD The Journal of Rheumatology SP 1040 OP 1047 DO 10.3899/jrheum.121507 VO 40 IS 7 A1 Iván Ferraz-Amaro A1 Miguel A. González-Gay A1 José A. García-Dopico A1 Federico Díaz-González YR 2013 UL http://www.jrheum.org/content/40/7/1040.abstract AB Objective. To investigate how cholesteryl ester transfer protein (CETP), one of the enzymes involved in the reverse cholesterol transfer, is expressed in patients with rheumatoid arthritis (RA) and its potential relationship with both dyslipidemia and the risk of cardiovascular mortality observed in these patients. Methods. Plasma CETP concentrations and CETP activity were measured in 101 patients with RA and 115 sex- and age-matched controls. A multivariable analysis adjusted for standard cardiovascular risk factors, including high-density lipoprotein cholesterol, was performed to evaluate the influence of CETP on dyslipidemia and cardiovascular mortality risk, as assessed by the Systematic Coronary Risk Evaluation (SCORE) risk function. Results. Patients with RA showed lower CETP activity [beta coefficient = −10.82 (95% CI −19.56 to 2.07) pmol/3 h; p = 0.02] and an inferior CETP mass [β = −0.85 (95% CI −1.64 to 0.05) μg/ml; p = 0.03] versus controls. Divided into those taking and those not taking glucocorticoids, patients taking glucocorticoids revealed lower CETP activity and mass [β = −8.98 (95% CI −14.55 to 3.41) pmol/3 h; p = 0.00, for CETP activity; and β = −0.77 (95% CI −1.46 to 0.08) μg/ml; p = 0.03, for CETP mass]. Patients with RA not taking glucocorticoids showed no differences versus controls in either CETP activity or mass. Both current prednisone intake [β = −16.14 (95% CI −24.87 to 7.41) pmol/3 h; p = 0.00] and average daily prednisone intake during the last 3 months [β = −0.36 (95% CI −0.54 to 0.18) μg/ml; p = 0.01] were strongly and inversely correlated with CETP activity and mass, respectively. CETP activity showed an inverse trend compared to SCORE risk, demonstrating that lower levels were effective predictors of total mortality when a higher SCORE risk was found [β = −4.7 (95% CI −9.3 to 0.02) pmol/3 h; p = 0.04] in patients with RA. Conclusion. CETP is downregulated in patients with RA who are taking glucocorticoids. Low CETP activity is associated with an increased level of cardiovascular risk in patients with RA.