Two-thirds of HIV-positive gay men with acute HCV achieve a good response to HCV therapy

Treatment for acute hepatitis C virus infection achieved a sustained virological response in almost two-thirds of HIV-positive gay men, according to data presented to the Third International Workshop on HIV and Hepatitis Coinfection in Paris on June 7^th.

Dr Sanjay Bhagani of London’s Royal Free Hospital, told delegates that 60% of patients with the ‘hard-to-treat’ hepatitis C genotype 1 achieved a sustained virological response. Patients whose baseline hepatitis C viralload was below 800,000 copies/ml and who had a rapid response (an undetectable hepatitis C viral load after four weeks of treatment) to therapy were most likely to experience successful treatment.

Outbreaks of hepatitis C have been reported amongst HIV-positive gay men in several European countries. It is thought that most of these men acquired the infection sexually. Because of increasing incidence of the infection in HIV-positive patients, and due to ongoing uncertainties about the best time to start hepatitis C therapy, and the duration of therapy, investigators in the UK, France and Germany formed a collaborative study in early 2007 to determine the risk factors, natural history and optimal treatment strategies for hepatitis C infection in HIV-positive individuals.

Preliminary retrospective data, collected from four treatment centres between 1999 and early 2006 were presented to the Paris workshop.

A total of 161 cases of acute hepatitis C were diagnosed in HIV-positive gay men at these centres. The average age was 38 years and sexual transmission was suspected in 88%, with 15% having a recent infection with syphilis. Most of the patients (93%) had their infection diagnosed due to abnormal liver function tests, but 17% were tested for hepatitis C infection because of the presence of symptoms.

Anti-hepatitis C therapy was initiated by 144 individuals and 131 completed this treatment. Data on these individuals were presented.

The majority of patients (70%) had the hard-to-treat genotype 1, with a further 10% having the equally difficult-to-treat genotype 4.

Potent anti-HIV therapy was being taken by 70% of patients, and immune function was well preserved in the study population, median CD4 cell count being 444 cells/mm³ and 80% of individuals had a viral load below 400 copies/ml. The initiation of anti-hepatitis C therapy caused a change of HIV therapy in 38% of patients.

In all, 74% of patients took what is now considered to be the standard of care for coinfected patients (pegylated-interferon plus ribavirin). Treatment was started within twelve weeks of hepatitis C being diagnosed in 57% of patients.

A total of 16% of individuals stopped therapy within 20 weeks, mostly because of intolerable side-effects. Most individuals (51%) took between 20 – 28 weeks of anti-hepatitis C treatment with 33% taking over 28 weeks therapy. Most of the patients who received longer duration of treatment received their care at the Royal Free Hospital in London.

A sustained virological response was achieved by 64% of patients overall, and by 60% of patients with genotype 1, a result which Dr Bhagani found highly encouraging.

Unsurprisingly, infection with genotypes 2/3 was associated with a higher odds ratio of a sustained virological response, as was treatment with a combination of pegylated-interferon and ribavirin. An undetectable hepatitis C viral load at weeks four and twelve predicted a sustained treatment response. Patients whose baseline hepatitis C viral load was below 800,000 copies/ml were also more likely to have a successful response to treatment. Receiving less than 20 weeks of therapy predicted poorer treatment response.

A blood disorder related to hepatitis C therapy was observed in 10% of patients and 13% experienced depression, a recognised side-effect of pegylated-interferon.