Direct-acting antiviral therapy for chronic hepatitis C virus genotype 4 infection: Exploring new regimens.

The optimal antiviral regimen for hepatitis C virus (HCV) genotype 4 is still a subject of investigation. The report in this issue of Health Science Reports by Asselah and colleagues investigated the additional benefit of extending treatment duration of the ombitasvir/paritaprevir/ritonavir plus ribavirin regimen to up to 24 weeks for patients with HCV genotype 4 and compensated cirrhosis.

The optimal antiviral regimen for hepatitis C virus (HCV) genotype 4 is still a subject of investigation. The report in this issue of Health Science Reports by Asselah and colleagues investigated the additional benefit of extending treatment duration of the ombitasvir/paritaprevir/ritonavir plus ribavirin regimen to up to 24 weeks for patients with HCV genotype 4 and compensated cirrhosis.
HCV genotype 4 accounts for over 8% of all patients with HCV infection globally. This genotype is predominantly found in patients from Egypt. Its prevalence varies widely by regions, with the highest prevalence reported in the Middle East and sub-Saharan Africa. 1 The geographic distribution of patients with HCV genotype 4 infection is increasing, however, due to migration. In Part II, reported in this issue, 5 two additional Arms were evaluated: Arm C, which included treatment-naïve patients or patients with a history of treatment with interferon/peginterferon plus ribavirin, and Arm D, which included patients with a history of sofosbuvir/ peginterferon plus ribavirin or sofosbuvir plus ribavirin. Patients were treated for 24 weeks in both Arms. The efficacy, tolerability, and safety were comparable across all four Arms. The extension of treatment duration to 24 weeks did not show superior efficacy to 12 or 16 weeks.
In addition, longer treatment duration did not offer additional benefit on short-term regression of liver fibrosis. These negative results are important for establishing the optimal regimen for patients with HCV genotype 4.
There is substantial genetic heterogeneity in HCV genotype 4, and many subgenotypes have been reported, although, with the exception of subtypes 4a and 4b, the prevalence of these subtypes is low. The efficacy of DAA regimens by subgenotype is unclear and will be the subject of further research. Although some trials that focused on patients with HCV genotype 4 have included more than of treatment failure in patients with HCV subgenotype 4r, a genotype which has been reported in African countries but that is rarely found in regions such as Europe and North America, which is associated with a high frequency of baseline resistance-associated substitutions.
Based on their report, it could be proposed that subgenotype evaluation should be recommended in patients with HCV genotype 4 when selecting a treatment regimen. However, given the low proportion of 4r in the overall HCV-infected population and the lack of available commercial assays to identify HCV genotype 4 subtypes, 9 universal subtyping of all genotype 4-infected patients to select regimen may be difficult to implement in actual clinical practice at this time.
The ideal DAA regimen for HCV genotype 4 has not been fully established, although there are multiple DAA treatment options for patients with HCV genotype 4, particularly those with the predominant subtypes, and overall efficacy in clinical trials has been reported to be as high as with other genotypes. We expect the accumulation of more findings on the efficacy of various regimens, and on different subtypes, perhaps based on real-world results, to confirm the high rates observed of sustained virologic response in patients with HCV genotype 4.

CONFLICTS OF INTEREST
None declared.