Hypercoagulability is a risk factor for cardiovascular events and D-dimers, which

are specific split products of fibrin degradation, represent a marker of activation and subsequent fibrinolysis. In the SMART study, increased D-dimers were associated with cardiovascular mortality selleck inhibitor [26], and a similar correlation was shown in a case–control study including HIV-infected patients enrolled in various National Institutes of Health (NIH)-initiated trials [38]. In the present study, D-dimers were significantly elevated in treatment-naïve patients, suggesting ongoing activation of coagulation and fibrinolysis. Treatment, however, reduced levels of D-dimers, as previously described [39]. Although our study suggests that antiretroviral treatment in the medium term improves markers of early vascular damage, selleck products it remains unclear whether the unfavourable alterations in, for example, lipid levels induced by HAART will outweigh this premature advantage in the long term. The PIs used at the initiation of HAART, indinavir and lopinavir, have both been associated with elevated CVD risk in the D : A : D study (4). In most Western countries these drugs are no longer in common use but have been replaced by newer drugs with less effect on lipids and presumably lower CVD risk. For this reason, the results of the present study may not be entirely representative

for the HIV-infected population of today. In addition, patients were not randomized to either NNRTI or PI, but treated sequentially. Therefore, the relative effects of the two drug classes cannot be assessed. We demonstrate that impaired endothelial function,

measured as FMD, and increased endothelial activation, inflammation and coagulation are present in untreated HIV-positive patients. These cardiovascular risk factors improved after the initiation of antiretroviral treatment, although not all parameters normalized after 6 months. Our results lend pathophysiological support to the finding of an increased risk of cardiovascular events in treatment-naïve HIV-infected patients. Treatment may reduce this risk by improving endothelial function, and reducing inflammation and vascular activation. Elevated lipid levels represent a risk factor induced by treatment; however, this risk depends on the drugs used. Our results support an overall beneficial effect of antiretroviral Liothyronine Sodium treatment on the risk of future cardiovascular events. This work was supported by The Danish AIDS Foundation, The Scandinavian Society of Antimicrobial Chemotherapy and The Research Council, University of Aarhus, Skejby, Denmark. “
“We recommend adherence and potential barriers to it are assessed and discussed with the patient whenever ART is prescribed or dispensed (GPP). We recommend adherence support should address both perceptual barriers (e.g. beliefs and preferences) and/or practical barriers (e.g. limitations in capacity and resources) to adherence (GPP).