The hepatitis D satellite virus of hepatitis B virus: half-opening a new era to control viral infection?

Curr Opin Infect Dis

aINSERM, U1052 UMR CNRS 5286, Centre de Recherches en Cancérologie de Lyon, Lyon, Cedex bUniversité Paris 13, UFR Santé Médecine Biologie Humaine cAssistance Publique-Hôpitaux de Paris, Groupe des Hôpitaux Universitaires Paris-Seine Saint Denis, Bobigny, France.

Published: December 2016

Purpose Of Review: To highlight new concepts and therapeutic approaches concerning hepatitis D virus (HDV) infection.

Recent Findings: Common receptor for hepatitis B virus (HBV) and HDV has been elucidated, deciphering of HDV replication is still in progress, preliminary results of phase II proof-of-concept clinical assays for entry inhibitors and cellular farnesyl transferase inhibitors are now available.

Summary: Hepatitis D infection remains a severe acute and chronic liver illness with the only currently approved therapy (Peg-αIFN) achieving disappointingly low rates of sustained viral response and clinical improvement. Both sodium taurocolate cotransporting polypeptide and heparan sulphate glypican 5 are important for viral adsorption. Preliminary results of 6 months treatment with a subcutaneous HBV PreS1-derived myristoyled peptide as an entry inhibitor indicates an encouraging short-term response with low side-effects. In addition, the short-term use of oral farnesyl transferase inhibitors induces a log10 reduction of viral RNA in almost all treated patients, but is associated with gastrointestinal upset and weight loss (especially using 200 mg/day). Encouraging results are being reported using intravenous phosphorothioate nucleic acid polymers both in terms of HBV surface antigens (HBsAg) and HDV-RNA decline; interestingly, in some patients with a strong HBsAg decline, the appearance of anti-hepatitis Bs antibodies might suggest clinical end-point improvement.

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Source
http://dx.doi.org/10.1097/QCO.0000000000000321DOI Listing

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