Demographics, presence of metabolic syndrome, alcohol use, laboratory data and clinical progression of liver disease were compared between the two groups using Student T-test, with statistical significance defined as p<0.05. Degree of fibrosis was assessed using FIB-4 and APRI, which were calculated
at time of HCV diagnosis and five years later. Cirrhosis was defined as evidence of nodularity by imaging. Results: The average age for the total population was 54.5 years, 52% were white, 94% male, and 78% overweight or obese (average BMI 29). No difference in tobacco use, or cholesterol levels was noted between the two groups. There were differences in alcohol consumption (p-value 0.013) and metabolic syndrome GSK3235025 chemical structure (p-value < 0.001) between the two cohorts. Five years after cohort entry, the cholecystectomy cohort was found to have increased rates of hepatic fibrosis, development of cirrhosis, ascites, hepatic encephalopathy, and death compared DZNeP price to the non- cholecystectomy cohort (Table 1). Importantly, absolute change in APRI (0.73) in the cholecystectomy cohort was different than then non-cholecystectomy cohort (0.36) (p-value 0.03). Conclusions: Cholecystectomy in patients with chronic HCV may be associated with increased rate of fibrosis, development of cirrhosis, ascites, hepatic encephalopathy and death compared to non-responder HCV patients. Disclosures: The following people have nothing to disclose: Donald J. Martin,
Rick A. Weideman, Terri Crook, Geri Brown Background: Liver-related deaths represent MCE公司 the leading cause of mortality among patients with HIV/HCV coinfection, and are mainly related to complications of fibrosis and portal hypertension (PHT). However, biomarkers for prediction of fibrosis progression and the degree of PHT in patients with HIV/HCV coinfection are currently not available. Thus, we assessed the value of extracellular matrix (ECM) degraded fragments in peripheral blood as biomarkers for fibrosis and PHT in HIV/
HCV coinfection. Methods: Fifty-eight patients (67% male, mean age: 36.5 years) with HIV/HCV coinfection were included in this study. Hepatic venous pressure gradient (HVPG) was measured in forty-three patients. The fibrosis stage was determined using the FIB4-Score. ECM degraded products (C4M, MMP-2/9 degraded type IV collagen; C5M, MMP-2/9 degraded type V collagen; PRO-C3, neoepitope specific propeptide of type III collagen formation) were measured in peripheral blood by ELISA PRO-C3 Results: HVPG showed strong and significant correlations with FIB4-Score (rs=0.628; p=7*10-7). PRO-C3 significantly correlated with HVPG (rs=0.354; p=0.02), alanine aminotransferase (rs=0.30; p=0.038), as well as with FIB4-Score (rs=0.3230; p=0.035). C4M and C5M levels were higher in patients with PHT. Conclusion: PRO-C3-levels reflecting true type III collagen formationcorrelated to hepatic injury, liver fibrosis stage, and PHT in HIV/HCV-co-infected patients.