Cardiovascular disease is the leading cause of death in patients with type 2 diabetes mellitus (T2DM). We suggested that plasma osteoprotegerin (OPG), a strong, independent predictor of cardiovascular disease, could discriminate between anti-diabetic treatments depending on their benefits regarding cardiovascular disease. The South Danish Diabetes Study, an investigator-driven, randomized, controlled clinical trial lasting 2 years, was used to test this hypothesis in patient groups with different medication strategies (insulin aspart or NPH insulin, added either metformin ⁄ placebo or rosiglitazone ⁄ placebo). A total of 371 individuals were eligible for the study. Basic variables were analysed along with measurement of plasma OPG and HbA 1c at the beginning and end of the study. Only rosiglitazone treatment caused a significant decrease in plasma OPG concentrations (p = 0.003), while no significant change was seen in the other treatment groups. The effect of rosiglitazone on plasma OPG remained significant in a univariate analysis adjusted for change in HbA 1c (p = 0.013). Of note, the change in plasma OPG significantly correlated with HbA 1c improvement in rosiglitazone-treated patients (R = 0.29, p = 0.0002), while this correlation was poor in those not receiving rosiglitazone (R = 0.06, p = 0.48). Treatment with rosiglitazone among patients with T2DM reduces the concentration of plasma OPG. This is not seen with metformin despite similar reductions in HbA 1c . Alteration in the OPG ⁄ RANKL pathway by glitazones may have implications for the understanding of both cardiovascular effects and bone side effects of the drug.Cardiovascular disease (CVD) is the leading cause of death in patients with type 2 diabetes mellitus (T2DM) [1,2]. Thus, a high number of diabetic patients suffer from heart disease, cerebrovascular disease or peripheral arterial disease [3][4][5]. Measures of glycaemic status correlate with and predict large vessel disease, and a meta-analysis has indicated that there may be beneficial effects of intensive glucose-lowering treatment on CVD events in diabetes, although this is debated [4,[6][7][8]. Reports have shown that peroxisome proliferatoractivated receptor (PPAR) c agonists (e.g. glitazones) in addition to their effects on insulin sensitivity improve some cardiovascular risk factors, e.g. blood pressure, coagulation factors and inflammation [9][10][11]. Moreover, experimental studies seem to indicate that activity of PPAR-c agonists is beneficial in relation to the atherogenic process. However, a recent meta-analysis has indicated that glitazones might be associated with an increased risk of myocardial infarction [12]. Recently, the final evaluation of the RECORD study revealed an increased risk of heart failure with the drug, but no increase in death from cardiac causes or all-cause mortality. Moreover, an increased risk of some fractures, mainly in women, was found when rosiglitazone was added to other glucose-lowering therapy in patients with T2DM compatible with other studi...
