All patients were to receive the combination of full-dose peginte

All patients were to receive the combination of full-dose peginterferon and ribavirin during the lead-in phase of the trial. Patients who remained viremic during the lead-in phase of treatment (lead-in patients), those who experienced virological breakthrough or this website relapse after initial response (breakthrough/relapser patients), and those who were nonresponders to peginterferon and ribavirin outside of the HALT-C trial (express patients) were randomized to maintenance therapy (peginterferon alpha-2a 90 μg weekly) or to remain as untreated controls for the next 3.5 years. Following completion

of the 3.5 years of the randomized trial, all patients were invited to continue follow-up without treatment until October 20, 2009. At entry, all patients were required to have an ultrasound, computed tomography (CT), or magnetic resonance imaging H 89 (MRI) demonstrating no evidence of hepatic mass lesions suspicious for HCC and to have an alpha fetoprotein (AFP) <200 ng/mL. All patients had a liver biopsy performed prior to enrollment. The Ishak scoring system was used to grade inflammation (0-18) and to stage fibrosis (0-6).13 The patients were seen every 3 months during the randomized phase of the trial and every 6 months thereafter. At each visit, patients were assessed clinically for outcomes and blood was drawn for complete blood count, hepatic panel (albumin, total bilirubin, aspartate aminotransferase [AST], alanine

aminotransferase [ALT], and alkaline phosphatase), creatinine, prothrombin time / international normalized ratio (INR), and AFP. Upper gastrointestinal endoscopy was performed at randomization to assess

for esophageal varices. Ultrasound was performed at randomization, 6 months after randomization, and then every 12 months during the randomized trial and every 6 months during the extended follow-up period. Patients with an elevated or rising AFP and those with new lesions on ultrasound were evaluated further with a CT or MRI. Diagnostic liver biopsy and HCC treatment were conducted at the discretion of investigators at each site. In this analysis, only patients randomized to no treatment were included because interferon even in low doses can have an effect on laboratory values. To assess changes in laboratory values Methocarbamol during follow-up, only patients who had been followed up to month 24 from enrollment (18 months after randomization to no treatment) with no outcomes up to that timepoint were included. Two clinical outcomes were analyzed: Outcome 1, Clinical decompensation, was defined as any of the following: variceal bleeding, ascites, spontaneous bacterial peritonitis, and hepatic encephalopathy; and Outcome 2, Liver-related deaths and liver transplantation. Diagnostic criteria were established for each clinical outcome and an Outcomes Review Panel adjudicated each outcome report. Only the first clinical outcome for each patient was included in this analysis.

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