Down-regulation of Viral Replication by Adenoviral-mediated Expression of SiRNA Against Cellular Cofactors for Hepatitis C Virus

Overview

Journal Virology

Specialty Microbiology

Date 2004 Mar 9

PMID 15003869

Citations 29

Authors

Jing Zhang

Osamu Yamada

Takashi Sakamoto

Hiroshi Yoshida

Takahiro Iwai

Yoshihisa Matsushita

Hideo Shimamura

Hiromasa Araki

Kunitada Shimotohno

Affiliations

Soon will be listed here.

Abstract

Small interfering RNA (siRNA) is currently being evaluated not only as a powerful tool for functional genomics, but also as a potentially promising therapeutic agent for cancer and infectious diseases. Inhibitory effect of siRNA on viral replication has been demonstrated in multiple pathogenic viruses. However, because of the high sequence specificity of siRNA-mediated RNA degradation, antiviral efficacy of siRNA directed to viral genome will be largely limited by emergence of escape variants resistant to siRNA due to high mutation rates of virus, especially RNA viruses such as poliovirus and hepatitis C virus (HCV). To investigate the therapeutic feasibility of siRNAs specific for the putative cellular cofactors for HCV, we constructed adenovirus vectors expressing siRNAs against La, polypyrimidine tract-binding protein (PTB), subunit gamma of human eukaryotic initiation factors 2B (eIF2Bgamma), and human VAMP-associated protein of 33 kDa (hVAP-33). Adenoviral-mediated expression of siRNAs markedly diminished expression of the endogenous genes, and silencing of La, PTB, and hVAP-33 by siRNAs substantially blocked HCV replication in Huh-7 cells. Thus, our studies demonstrate the feasibility and potential of adenoviral-delivered siRNAs specific for cellular cofactors in combating HCV infection, which can be used either alone or in combination with siRNA against viral genome to prevent the escape of mutant variants and provide additive or synergistic anti-HCV effects.

Citing Articles

Xue J, Cheng J, Ma X, Shi Y, Yin H, Gao Y J Clin Transl Hepatol. 2021; 9(4):458-465.

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Model of OSBP-Mediated Cholesterol Supply to Aichi Virus RNA Replication Sites Involving Protein-Protein Interactions among Viral Proteins, ACBD3, OSBP, VAP-A/B, and SAC1.

Ishikawa-Sasaki K, Nagashima S, Taniguchi K, Sasaki J J Virol. 2018; 92(8).

PMID: 29367253 PMC: 5874406. DOI: 10.1128/JVI.01952-17.

Combinations of siRNAs against La Autoantigen with NS5B or hVAP-A Have Additive Effect on Inhibition of HCV Replication.

Mandal A, Ganta K, Chaubey B Hepat Res Treat. 2016; 2016:9671031.

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MEAN inhibits hepatitis C virus replication by interfering with a polypyrimidine tract-binding protein.

Xue J, Liu Y, Yang Y, Wu S, Hu Y, Yang F J Cell Mol Med. 2016; 20(7):1255-65.

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Zhang J, Yamada O, Kida S, Matsushita Y, Hattori T Cell Oncol (Dordr). 2015; 39(2):119-28.

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