Identification of a novel interaction site between the large hepatitis delta antigen and clathrin that regulates the assembly of genotype III hepatitis delta virus

Wei-Chung Chiou; Hsu-Feng Lu; Jui-Chieh Chen; Yu-Heng Lai; Ming-Fu Chang; Yuan-Li Huang; Ni Tien; Cheng Huang

doi:10.1186/s12985-022-01866-3

Virology Journal (Oct 2022)

Identification of a novel interaction site between the large hepatitis delta antigen and clathrin that regulates the assembly of genotype III hepatitis delta virus

Wei-Chung Chiou,
Hsu-Feng Lu,
Jui-Chieh Chen,
Yu-Heng Lai,
Ming-Fu Chang,
Yuan-Li Huang,
Ni Tien,
Cheng Huang

Affiliations

Wei-Chung Chiou: Department of Biotechnology and Laboratory Science in Medicine, National Yang Ming Chiao Tung University
Hsu-Feng Lu: Department of Medical Laboratory Science and Biotechnology, Asia University
Jui-Chieh Chen: Department of Biochemical Science and Technology, National Chiayi University
Yu-Heng Lai: Department of Chemistry, Chinese Culture University
Ming-Fu Chang: Institute of Biochemistry and Molecular Biology, School of Medicine, National Taiwan University
Yuan-Li Huang: Department of Medical Laboratory Science and Biotechnology, Asia University
Ni Tien: Department of Laboratory Medicine, China Medical University Hospital
Cheng Huang: Department of Biotechnology and Laboratory Science in Medicine, National Yang Ming Chiao Tung University

DOI: https://doi.org/10.1186/s12985-022-01866-3
Journal volume & issue: Vol. 19, no. 1
pp. 1 – 9

Abstract

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Abstract Background Hepatitis delta virus (HDV), a satellite virus of hepatitis B virus (HBV), is a small, defective RNA virus strongly associated with the most severe form of hepatitis and progressive chronic liver disease and cirrhosis. Chronic hepatitis D, resulting from HBV/HDV coinfection, is considered to be the most severe form of viral hepatitis and affects 12–20 million people worldwide. Involved in the endocytosis and exocytosis of cellular and viral proteins, clathrin contributes to the pathogenesis and morphogenesis of HDV. Previously, we demonstrated that HDV-I and -II large hepatitis delta antigens (HDAg-L) possess a putative clathrin box that interacts with clathrin heavy chain (CHC) and supports HDV assembly. Methods Virus assembly and vesicular trafficking of HDV virus-like particles (VLPs) were evaluated in Huh7 cells expressing HDV-I, -II and -III HDAg-L and hepatitis B surface antigen (HBsAg). To elucidate the interaction motif between HDAg-L and CHC, site-directed mutagenesis was performed to introduce mutations into HDAg-L and CHC and analyzed using coimmunoprecipitation or pull-down assays. Results Comparable to HDV-I virus-like particles (VLPs), HDV-III VLPs were produced at a similar level and secreted into the medium via clathrin-mediated post-Golgi vesicular trafficking. Mutation at F27 or E33 of CHC abolished the binding of CHC to the C-terminus of HDV-III HDAg-L. Mutation at W207 of HDV-III HDAg-L inhibited its association with CHC and interfered with HDV-III VLP formation. We elucidated mechanism of the binding of HDV-III HDAg-L to CHC and confirmed the pivotal role of clathrin binding in the assembly of genotype III HDV. Conclusions A novel W box which was identified at the C terminus of HDV-III HDAg-L is known to differ from the conventional clathrin box but also interacts with CHC. The novel W box of HDAg-L constitutes a new molecular target for anti-HDV-III therapeutics.

Published in Virology Journal

ISSN: 1743-422X (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine: Infectious and parasitic diseases
Website: http://virologyj.biomedcentral.com

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