Because this work associates secondary prophylaxis with longer survival in HCC patients who bled from varices, this treatment measure should not be forgotten. (Hepatology 2013;58:2079-2088.) “
“We read with great interest the article by Kim et al. about the association between nonalcoholic fatty liver disease (NAFLD) and coronary artery calcification (CAC). Crizotinib mw The authors concluded that NAFLD per se might be a risk factor for coronary artery disease (CAD) as the association was “above and beyond visceral adiposity
(VAT).”1 Interestingly, the Framingham Heart Study showed that VAT, body mass index, and pericardial fat (PCF) are associated with CAC, but only PCF remains significant following risk factor Small molecule library order adjustment, suggesting a locally toxic effect of PCF on the vasculature.2 Thus, Kim et al. still leave open a key question about whether the contribution of NAFLD to CAC is above and beyond PCF. That would be an interesting hypothesis to test, even though the current evidence linking NAFLD, carotid artery wall thickness, and plaque development strongly suggests so.3 The authors also suggested that the pathogenesis of the association between NAFLD and CAD has not been thoroughly investigated. We would like to add
some comments, as we have shown that the contribution of NAFLD to a proatherogenic profile is biologically plausible (Fig. 1), and the atherogenic risk is related to the disease severity. The liver of nonalcoholic steatohepatitis patients showed overexpression of proatherogenic genes such as TGFB1,4 which is associated with a high incidence of coronary events and restenosis after coronary intervention. NAFLD might also participate in the pathogenesis of CAD through the release of molecular mediators of atherogenesis such as sICAM-1, PAI-1, and sCD40L.5 Accordingly,
patients with NAFLD showed higher liver expression of ICAM-1 and PAI-1, and a significant correlation was found between both the Ureohydrolase degree of liver steatosis and the severity of necroinflammatory activity and liver ICAM-1 expression.5 This scenario suggests that NAFLD participates in the crosstalk with target organs, leading to vascular disease and causing a change in the classical paradigm about the role of local versus distant toxic fat accumulation and deleterious vascular effects. Thus, all of us should take notice of the potential secretory/endocrine role of the fatty liver and its impact on the modulation of systemic phenotypes. This study was partially supported by grants PICT 2008-1521 and 2010-0441 (Agencia Nacional de Promoción Científica y Tecnológica), and UBACYT CM04 (Universidad de Buenos Aires). Silvia Sookoian M.D., Ph.D.* , Gustavo O. Castaño M.D., Ph.D., Carlos J. Pirola Ph.D.