Alexander Tonthat scite author profile

Chronic hepatitis B virus (HBV) infection remains difficult to cure due to the persistent, self‐replenishing nature of the viral genome and impaired host immune responses. Current treatment goals for chronic hepatitis B (CHB) are to prevent or significantly delay liver‐related adverse outcomes and death, and two types of treatments are available: nucleos(t)ide analogues (NAs) and interferons (IFNs). NAs effectively suppress HBV replication, and IFNs improve serological response rates, thereby decreasing the risk of adverse outcomes. However, their efficacy in attaining serological responses, especially functional cure (i.e., loss of serum hepatitis B surface antigen), is very limited. Various strategies such as stopping antiviral therapy or combining therapies have been investigated to enhance response, but efficacy is only modestly improved. Importantly, the development of novel direct‐acting antivirals and immunomodulators is underway to improve treatment efficacy and enhance rates of functional cure. The present review provides an overview of the treatment goals and indications, the possibility of expanding indications, and the safety and efficacy of different treatment strategies involving established and/or novel therapies as we continue our search for a cure.

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Recent use of NSAID and NOAC medications are associated with a positive CT arteriogram

Shafqet

Tonthat

Esparragoza

et al. 2019

Abdom Radiol

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Editorial: risk of hepatocellular carcinoma with tenofovir vs entecavir—a “knock‐out” is yet to be delivered

Tonthat

Zhou

2022

Aliment Pharmacol Ther

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Su1473 PREDICTORS OF DIABETES MELLITUS FOLLOWING DISCHARGE FOR ACUTE PANCREATITIS

Hiramoto¹,

Buitrago²,

Hilson³

et al. 2020

Gastroenterology

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Mo1026 YIELD OF OUTPATIENT ENDOSCOPY FOR DYSPEPSIA IN A HIGH-RISK POPULATION FOR GASTRIC CANCER

Tonthat¹,

Bernardo²,

Buxbaum³

et al. 2020

Gastroenterology

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