19 [112-127], P < 00001) and SF greater than 500 μg/L (HR 105

19 [1.12-1.27], P < 0.0001) and SF greater than 500 μg/L (HR 10.52 [2.88-38.43], P < 0.0001) were associated with increased 180-day mortality (Table 3). In univariate analysis, the following factors were associated with 1-year mortality: SF greater than 500 μg/L (HR 11.05 [3.33-36.7], P < 0.0001), MELD (HR 1.15 [1.10-1.21], P < 0.0001), serum sodium concentration less than 126 μmol/L (HR 4.80 [1.54-15.02], P = 0.007), and serum sodium concentration

less than 131 μmol/L (HR 2.81 [1.16-6.80], P = 0.02). After multivariate analysis, MELD (HR 1.20 [1.12-1.27], P < 0.0001) and SF greater than YAP-TEAD Inhibitor 1 research buy 500 μg/L (HR 14.39 [4.10-50.47], P < 0.0001) were associated with increased 1-year mortality (Table 4). ROC curve analysis of mortality in the UCLA cohort showed the addition of SF to MELD increased the area under the ROC curve for

180-day and 1-year mortality by 21.4% (0.7-0.86, P = 0.001) and 40.3% (0.63-0.87, P < 0.0001), respectively. In contrast to the study population, there was no increase in the area under the ROC curve for 180-day and 1-year mortality when serum sodium was added to MELD and SF. Within two decades, liver transplantation has evolved from a novel treatment option conducted in a few major centers to a widely available and highly successful therapy for advanced liver disease. Simultaneous with the development of OLT, there has been a dramatic increase AZD0530 research buy in the burden of liver disease in the community largely because of hepatitis C and obesity epidemics. Epidemiological studies predicting the future burden of liver disease suggest that incident cases of liver failure and HCC will double by 2020.4 Therefore, the number of patients requiring

OLT is likely to increase. Unless there is a commensurate increase in organ donation, the number of patients on liver transplant waiting lists and waiting list mortality will rise, as is already occurring in some parts of the world.15 A further effect of increased number of patients on waiting lists is that many prospective recipients will have an identical MELD and organ allocation 上海皓元 in this circumstance may return to decisions based on subjective criteria. Thus, it is important to identify objective prognostic markers that can be used in conjunction with MELD to maintain appropriate strategies for liver allocation and minimize deaths on the liver transplant waiting list. Serum ferritin concentration is a widely available and objective laboratory parameter. In this study, we showed that SF provided important prognostic information—independent of MELD and the presence of HCC—in predicting 180-day and 1-year OLT waiting list mortality in adult patients with cirrhosis. This relationship between SF and liver transplant waiting list mortality was identified in a study cohort of Australian patients, and these findings were confirmed in an analysis of patients from UCLA Transplant Center, California.

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