5, 6 In the present study, adiponectin levels were not significantly elevated in those with advanced-stage NASH fibrosis/cirrhosis when compared to those with early disease. One might have expected the levels to be lower in patients with advanced NASH who were more insulin resistant and obese
than those with early disease, but it is established that adiponectin Selleck Opaganib levels in cirrhosis do not correlate with insulin resistance, dyslipidemia, or obesity.17, 18 The unaltered levels of adiponectin in late compared to early disease is in part a deliberate consequence of our strict selection criteria, wherein we excluded (1) all patients with markers of liver synthetic dysfunction such as abnormal prothrombin time, albumin, or bilirubin, and (2) those with Child’s B and C cirrhosis. Thus, we were able to exclude elevations due to these confounders
known to be associated with increased adiponectin, and further strengthen our hypothesis.17, 18 Adiponectin levels are also lower in patients with nonalcoholic fatty liver disease (NAFLD) compared to other liver diseases29 and levels decline further with increasing necroinflammation and fibrosis. Thus, the finding of similar adiponectin levels for our two groups is in keeping with a www.selleckchem.com/screening/tyrosine-kinase-inhibitor-library.html relative elevation of adiponectin, similar to that seen in other forms of cirrhosis. Taken together, these findings suggest that physiological regulation of adiponectin selleck is dramatically altered in patients with advanced-stage liver disease compared to the situation in healthy volunteers, diabetes, or early liver disease.16, 30 A number of mechanisms have been hypothesized to explain the relative elevation in adiponectin with progressive fibrosis, including an imbalance between adiponectin production and hepatic extraction,18, 31 a protective antiinflammatory mechanism in the chronic inflammatory
state of cirrhosis,18 and an increase in true hepatocyte or hepatic stellate cell adiponectin production.17, 32 Because the highest levels of adiponectin are seen in patients with advanced cholestatic liver disease, reduced biliary excretion of adiponectin may also be important.15, 17, 33 This theory is supported by bile duct ligation studies in mice where dramatic increases in serum adiponectin were seen over time, and the detection of adiponectin in the bile of human subjects with severe cholestasis.15 None of the patients included in this study were severely catabolic or clinically had cholestasis (elevations in bilirubin), which raised the intriguing question as to why adiponectin would be elevated in our cohort and whether there could be a link between hepatocyte dysfunction and adiponectin production by adipose tissues.