AI Article Synopsis
- HPgV NS3 protease has been found to inhibit HIV replication in CD4+ T cells while also being similar to the HCV NS3 protease.
- Researchers investigated whether HPgV protease affects type I interferon responses or is impacted by HCV protease inhibitors and found that major HCV inhibitors do not affect HPgV activity.
- The study revealed that HPgV NS3 protease can cleave MAVS and inhibit interferon responses, potentially promoting HPgV persistence, which may provide clinical benefits for HIV-infected patients.
Article Abstract
We previously found that human pegivirus (HPgV; formerly GBV-C) NS3 protease activity inhibits Human Immunodeficiency Virus (HIV) replication in a CD4+ T cell line. Given the protease׳s similarity to the Hepatitis C virus (HCV) NS3 protease, we characterized HPgV protease activity and asked whether it affects the type I interferon response or is inhibited by HCV protease antagonists. We characterized the activity of proteases with mutations in the catalytic triad and demonstrated that the HCV protease inhibitors Telaprevir, Boceprevir, and Danoprevir do not affect HPgV protease activity. HPgV NS3 protease cleaved MAVS but not TRIF, and it inhibited interferon responses sufficiently to enhance growth of an interferon-sensitive virus. Therefore, HPgV׳s inhibition of the interferon response could help promote HPgV persistence, which is associated with clinical benefits in HIV-infected patients. Our results also imply that HCV protease inhibitors should not interfere with the beneficial effects of HPgV in HPgV/HCV/HIV infected patients.
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| http://dx.doi.org/10.1016/j.virol.2014.03.018 | DOI Listing |
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