Pioglitazone improves the cardiovascular profile in patients with uncomplicated systemic lupus erythematosus: a double-blind randomized clinical trial

Author:

Juárez-Rojas JG12,Medina-Urrutia AX1,Jorge-Galarza E1,Caracas-Portilla NA1,Posadas-Sánchez R1,Cardoso-Saldaña GC1,Goycochea-Robles MV3,Silveira LH4,Lino-Pérez L5,Mas-Oliva J6,Pérez-Méndez O7,Posadas-Romero C1

Affiliation:

1. Endocrinology Department, National Institute of Cardiology “Ignacio Chávez”, Mexico

2. Doctorate Program of Biomedical Sciences from the National Autonomous University of Mexico, Mexico

3. Clinical Epidemiology Research Unit, Number 1 Regional Hospital from the Mexican Institute of the Social Security, Carlos McGregor Sánchez Navarro, Mexico

4. Rheumatology Department, National Institute of Cardiology “Ignacio Chávez”, Mexico

5. Rheumatology Department, Mexican General Hospital, Mexico

6. Cellular Physiology Institute, National Autonomous University of Mexico, Mexico

7. Molecular Biology Department, National Institute of Cardiology “Ignacio Chávez”, Mexico

Abstract

Objective: We studied the effect of pioglitazone on insulin levels, inflammation markers, high-density lipoprotein (HDL) composition and subclasses distribution, in young women with uncomplicated systemic lupus erythematosus (SLE). Methods: This double-blind trial included 30 premenopausal women (30 ±8 years old) with SLE, who were randomized to pioglitazone (30 mg/day) or placebo treatment for 3 months. Plasma and HDL lipids were determined by colorimetric enzymatic assays, insulin by radioimmunometric assay, inflammation by immunonephelometry and HDL size and subclasses distribution by a native 4–30% polyacrylamide gradient gel electrophoresis. Results: Compared with placebo, pioglitazone significantly increased HDL-cholesterol plasma levels (14.2%), reduced fasting insulin plasma levels (23.6%) and the homeostasis model assessment-insulin resistance (31.7%). C-reactive protein (70.9%) and serum amyloid A (34.9%) were also significantly reduced with the pioglitazone use, whereas the HDL particle size was increased (8.80 nm vs. 8.95 nm; p = 0.044) by changes in the distribution of HDL2b, HDL3b, and HDL3c subclasses. The change in HDL size correlated with a rise in free and cholesterol–ester content in the HDL particles. Conclusion: Pioglitazone significantly enhanced insulin sensitivity, reduced inflammation, and modified HDL characteristics, suggesting a potential beneficial effect of this drug in patients with SLE with a risk to develop cardiovascular disease. Trial registration: This trial is registered at ClinicalTrials.gov Protocol Registration System, with the number NCT01322308.

Publisher

SAGE Publications

Subject

Rheumatology

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