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Literature DB >> 23391846

Chronic hepatitis B: what should be the goal for new therapies?

Timothy M Block¹, Robert Gish, Haitao Guo, Anand Mehta, Andrea Cuconati, W Thomas London, Ju-Tao Guo.

Abstract

Chronic hepatitis B can currently be medically managed with either pegylated interferon-alpha (pegIFN-α) or one of the five nucleos(t)ide analog Direct Acting Antivirals (DAAs) that inhibit the hepatitis B virus (HBV) DNA polymerase. While pegIFN-α is effective in approximately one-third of the treated patients, the polymerase inhibitors significantly reduce viral load in the vast majority of those treated. However, neither pegIFN-α nor nucleosi(t)de analogs are capable of reliably eliminating the virus and achieving a cure. Moreover, the interferons and polymerase inhibitors are recommended by US, European and Asian professional society practice guidelines for use in only a subset of those infected with HBV. This subset is the population with the greatest levels of circulating viral DNA and abnormal liver function. Although this is the population at the highest risk for cirrhosis and liver cancer, those who fall outside the treatment guidelines, with low levels of viral replication and normal serum ALTs, may also benefit from antiviral therapy. The questions are thus: are new classes of drugs needed to manage chronic hepatitis B? Is a cure possible? Is a cure even necessary? It is therefore important to define the meaning of a cure and determine what the goals of new therapies should be. In this article, we address those questions and propose two operational definitions of medically attainable cures. The first is a "functional cure" based on the clinical outcome, in which the patient's life expectancy becomes the same as that of an individual who has resolved his HBV infection without therapy. Because such an outcome cannot be measured over the short term, we also define an "apparent virological cure," based on the stable off-drug suppression of HBV viremia and antigenemia and the normalization of ALTs and other laboratory tests. We suggest that such a virological cure should be the goal of future therapeutics in all patients with chronic hepatitis B. The extent to which a virological cure predicts a functional cure will only be determined by long-term follow-up.

Entities: CellLine Chemical Disease Gene Species

Mesh：

Substances：
Antiviral Agents

Year: 2013 PMID： 23391846 PMCID： PMC3627746 DOI： 10.1016/j.antiviral.2013.01.006

Source DB: PubMed Journal: Antiviral Res ISSN： 0166-3542 Impact factor: 5.970

70 in total

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Journal: Gastroenterology Date: 2010-04-24 Impact factor: 22.682

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Journal: Hepatology Date: 2009-04 Impact factor: 17.425

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Journal: Aliment Pharmacol Ther Date: 2008-07-24 Impact factor: 8.171

54 in total

Review 1. Metabolism and function of hepatitis B virus cccDNA: Implications for the development of cccDNA-targeting antiviral therapeutics.

Authors: Ju-Tao Guo; Haitao Guo
Journal: Antiviral Res Date: 2015-08-10 Impact factor: 5.970

2. Hepatitis B virus replication is blocked by a 2-hydroxyisoquinoline-1,3(2H,4H)-dione (HID) inhibitor of the viral ribonuclease H activity.

Authors: Catherine W Cai; Elena Lomonosova; Eileen A Moran; Xiaohong Cheng; Kunjan B Patel; Fabrice Bailly; Philippe Cotelle; Marvin J Meyers; John E Tavis
Journal: Antiviral Res Date: 2014-05-20 Impact factor: 5.970

3. Characterization of novel hepadnaviral RNA species accumulated in hepatoma cells treated with viral DNA polymerase inhibitors.

Authors: Pinghu Zhang; Fei Liu; Fang Guo; Qiong Zhao; Jinhong Chang; Ju-Tao Guo
Journal: Antiviral Res Date: 2016-04-12 Impact factor: 5.970

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Authors: Juan Antonio Villa; Daniel P Pike; Kunjan B Patel; Elena Lomonosova; Gaofeng Lu; Roz Abdulqader; John E Tavis
Journal: Antiviral Res Date: 2016-06-17 Impact factor: 5.970

10. Hepatitis B Virus Polymerase Localizes to the Mitochondria, and Its Terminal Protein Domain Contains the Mitochondrial Targeting Signal.

Authors: Nuruddin Unchwaniwala; Nathan M Sherer; Daniel D Loeb
Journal: J Virol Date: 2016-09-12 Impact factor: 5.103