Several investigations have been published on Hepatitis Delta Virus (HDV) infection in recent years, from which we have drawn the salient data to provide readers with useful information to improve their knowledge on the subject. HDV genotypes 5–8 have been recently imported to Western countries from central Africa, whose clinical relevance deserves further investigation. On-going HDV replication has been identified as an independent predictor of progression to cirrhosis and HCC for patients with HDV chronic hepatitis (HDV‐CH). Long‐term treatments of HDV‐CH with standard or pegylated interferon alfa (peg‐IFN‐α) have all been unsatisfactory, leading to a sustained virological response (SVR) only in 20–30% of patients treated, faced with a poor tolerabil-ity and frequent serious adverse reactions; the addition of HBV nucleo(s)tide analogues to peg‐IFN-α did not improve the rate of SVR. The improved knowledge of the HDV life cycle has allowed the development of direct acting agents towards key‐points of the HDV life cycle, namely bulevirtide, lonafarnib and nucleic acid polymers. Preliminary data have shown that these drugs are more effective than interferon‐based therapies, but adverse reactions are also common, which however seem toned down in combination therapy with other antivirals.

Hbv/hdv co‐infection: Epidemiological and clinical changes, recent knowledge and future challenges

Sagnelli C.;Sagnelli E.;Russo A.;Pisaturo M.;Coppola N.
2021

Abstract

Several investigations have been published on Hepatitis Delta Virus (HDV) infection in recent years, from which we have drawn the salient data to provide readers with useful information to improve their knowledge on the subject. HDV genotypes 5–8 have been recently imported to Western countries from central Africa, whose clinical relevance deserves further investigation. On-going HDV replication has been identified as an independent predictor of progression to cirrhosis and HCC for patients with HDV chronic hepatitis (HDV‐CH). Long‐term treatments of HDV‐CH with standard or pegylated interferon alfa (peg‐IFN‐α) have all been unsatisfactory, leading to a sustained virological response (SVR) only in 20–30% of patients treated, faced with a poor tolerabil-ity and frequent serious adverse reactions; the addition of HBV nucleo(s)tide analogues to peg‐IFN-α did not improve the rate of SVR. The improved knowledge of the HDV life cycle has allowed the development of direct acting agents towards key‐points of the HDV life cycle, namely bulevirtide, lonafarnib and nucleic acid polymers. Preliminary data have shown that these drugs are more effective than interferon‐based therapies, but adverse reactions are also common, which however seem toned down in combination therapy with other antivirals.
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11591/462434
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