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Many hepatitis C patients with cirrhosis or advanced fibrosis face liver failure and liver cancer
Liz Highleyman, 2014-12-18 07:10:00

Nearly one-third of chronic hepatitis C patients with liver cirrhosis and 12% with advanced fibrosis progressed to decompensation within five years, and 23% and 11%, respectively, died, according to a study presented at the American Association for the Study of Liver Diseases (AASLD) Liver Meeting last month in Boston. These findings underscore the urgent need for treatment for such individuals.

Over years or decades chronic hepatitis C virus (HCV) infection can progress to serious liver disease including cirrhosis, hepatocellular carcinoma (HCC), liver decompensation -- when the liver can no longer carry out its vital functions -- and liver-related death.

Successful treatment that leads to sustained virological response (SVR) can slow or halt liver disease progression and may allow for some degree of recovery. When the standard of care was interferon-based therapy -- which lasted up to a year, caused difficult side effects and cured only about half of patients -- treatment was recommended only for people with evidence of progressive liver damage.

Now that highly effective and well-tolerated interferon-free direct-acting antiviral regimens are available, some experts have called for universal treatment. But given the drugs' high cost, current guidelines state that people with advanced liver disease should be prioritised, and many national health systems and private insurers are limiting treatment to the sickest patients.

Anne Moorman from the U.S. Centers for Disease Control and Prevention and colleagues looked at liver disease progression to decompensation or HCC and all-cause mortality among patients in the Chronic Hepatitis Cohort Study. CHeCS is an ongoing observational study of more than 14,000 hepatitis C patients at four integrated healthcare systems in Michigan, Pennsylvania, Hawaii and Oregon.

This analysis included 2,839 chronic hepatitis C patients with biopsy-confirmed fibrosis in the era prior to direct-acting antivirals. Participants had liver biopsies performed during 2001-2012, before the onset of HCC or decompensation, and before receiving hepatitis C treatment.

A majority of participants (about 60%) were men, two-thirds were white and the median age was just over 50 years; more than 80% were in the highest-risk 1945-1965 birth cohort. Baseline biopsies revealed that 1,204 (42%) had absent or mild fibrosis (Metavir stage F0-F1), 810 (29%) had moderate fibrosis (stage F2), 461 (16%) had advanced fibrosis (stage F3) and 364 had cirrhosis (stage F4).

The researchers analysed the number of cases of HCC, decompensation, liver transplantation and death due to all causes over an average follow-up period of 5.5 years. Decompensation was defined as the first occurrence of portal hypertension, ascites (abdominal fluid accumulation), oesophageal varices (distended veins), hepatic encephalopathy (brain impairment) or liver failure with hepato-renal syndrome.

Among people with cirrhosis at baseline, 29% experienced decompensation, 11% developed HCC, 5% underwent liver transplantation and 23% died due to any cause. Among people with advanced fibrosis, 12% experienced decompensation, 5% developed HCC, 2% had transplants and 11% died. Among people with moderate fibrosis, the rates were lower: 4%, 1%, 1% and 6%, respectively.

Looking at treatment, 62% of participants with cirrhosis, 72% with advanced fibrosis and 46% with moderate fibrosis were ever treated after their baseline biopsy. Among the subset of patients with known treatment outcomes, 47%, 55% and 75%, respectively, achieved sustained virological response.

Among people with cirrhosis, the risk of decompensation was significantly lower among treated compared with untreated patients -- approximately 25% vs 50% at the maximum follow-up of seven years; the risk of HCC was also significantly lower, about 7% vs 15%.

Among people with stage F3 fibrosis, the difference in decompensation rates between treated and untreated patients was also significant, 10% vs 25% at seven years. Fewer treated patients developed HCC (approximately 4% vs 7%), but this difference did not reach statistical significance.

There was no significant difference in decompensation or HCC rates between treated and untreated patients with F2 fibrosis, but rates were low -- under 4% for decompensation and under 2% for HCC -- in both groups.

In a multivariate analysis, people with cirrhosis were about five times more likely to experience decompensation, and those with F3 fibrosis were nearly three times more likely, compared to those with F2 fibrosis. Low platelet count and elevated bilirubin at baseline were also associated with a greater risk of decompensation, while receiving treatment was associated with a 30% lower risk.

"We observed substantial liver disease progression in a population-based observational cohort among patients meeting liver disease stage criteria that now confer 'high' or 'highest' recommendation for treatment," the researchers concluded.

These findings show that people with advanced fibrosis, in addition to those with cirrhosis, are at substantial risk of liver-related complications as should receive treatment. People with moderate fibrosis are at lower risk, but still four out of 100 may progress to decompensation without treatment.

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