Hepatitis B Virus Therapeutic Agent ARB-1740 Has Inhibitory Effect on Hepatitis Delta Virus in a New Dually-Infected Humanized Mouse Model

Overview

Journal ACS Infect Dis

Specialties Infectious Diseases
Microbiology
Pharmacology

Date 2018 Nov 10

PMID 30408957

Citations 14

Authors

Xin Ye

Chise Tateno

Emily P Thi

Masakazu Kakuni

Nicholas M Snead

Yuji Ishida

Trisha R Barnard

Michael J Sofia

Takashi Shimada

Amy C H Lee

Affiliations

Soon will be listed here.

Abstract

Hepatitis delta virus (HDV) infects 10-20 million individuals worldwide and causes severe fulminant hepatitis with high likelihood of cirrhosis and hepatocellular carcinoma. HDV infection cannot occur in the absence of the surface antigen (HBsAg) of the hepatitis B virus. RNA interference is an effective mechanism by which to inhibit viral transcripts, and siRNA therapeutics sharing this mechanism have begun to demonstrate clinical efficacy. Here we assessed the outcome of HBV-targeting siRNA intervention against HDV and compared it to a direct anti-HDV siRNA approach in dually infected humanized mice. Treatment with ARB-1740, a clinical stage HBV-targeting siRNA agent delivered using lipid nanoparticle (LNP) technology, effectively reduced HBV viremia by 2.3 log and serum HBsAg by 2.6 log, leading to 1.6 log reduction of HDV viremia. In contrast, HDV-targeting siRNA inhibited HDV in both blood and liver compartments without affecting HBV and PEGylated interferon-alpha reduced HBV viremia by 2.0 log but had no effect on HDV viremia under these study conditions. These results illustrate the inhibitory effects of siRNAs against these two viral infections and suggest that ARB-1740 may be of therapeutic benefit for hepatitis delta patients, a subpopulation with high unmet medical need.

Citing Articles

Preclinical testing of antiviral siRNA therapeutics delivered in lipid nanoparticles in animal models - a comprehensive review.

Idres Y, Idris A, Gao W Drug Deliv Transl Res. 2025; .

PMID: 40000558 DOI: 10.1007/s13346-025-01815-x.

Evaluation of Interfering RNA Efficacy in Treating Hepatitis B: Is It Promising?.

Angelice G, Roque P, Valente G, Galvao K, Villar L, Mello V Viruses. 2024; 16(11).

PMID: 39599825 PMC: 11598949. DOI: 10.3390/v16111710.

Lipid-nanoparticle-enabled nucleic acid therapeutics for liver disorders.

Arjunan P, Kathirvelu D, Mahalingam G, Goel A, Zacharaiah U, Srivastava A Acta Pharm Sin B. 2024; 14(7):2885-2900.

PMID: 39027251 PMC: 11252464. DOI: 10.1016/j.apsb.2024.04.015.

Gene-Editing and RNA Interference in Treating Hepatitis B: A Review.

Kasianchuk N, Dobrowolska K, Harkava S, Bretcan A, Zarebska-Michaluk D, Jaroszewicz J Viruses. 2023; 15(12).

PMID: 38140636 PMC: 10747710. DOI: 10.3390/v15122395.

Ionizable drug delivery systems for efficient and selective gene therapy.

Zhang Y, Guo R, Chen Y, Li T, Du W, Xiang R Mil Med Res. 2023; 10(1):9.

PMID: 36843103 PMC: 9968649. DOI: 10.1186/s40779-023-00445-z.