Efficient Inhibition of Hepatitis B Virus Infection by a PreS1-binding Peptide

Overview

Journal Sci Rep

Specialty Science

Date 2016 Jul 8

PMID 27384014

Citations 9

Authors

Xiaoli Ye

Ming Zhou

Yonggang He

Yanmin Wan

Weiya Bai

Shuai Tao

Yanqin Ren

Xinxin Zhang

Jianqing Xu

Jing Liu

Junqi Zhang

Kanghong Hu

Youhua Xie

Affiliations

Soon will be listed here.

Abstract

Entry inhibitors are promising novel antivirals against hepatitis B virus (HBV) infection. The existing potential entry inhibitors have targeted the cellular receptor(s). In this study, we aim to develop the first entry inhibitor that inhibits HBV infection via targeting viral particles. The preS1 segment of the large envelope glycoprotein of HBV is essential for virion attachment and infection. Previously, we obtained a preS1-binding short peptide B10 by screening a phage display peptide library using the N-terminal half of preS1 (residues 1 to 60, genotype C). We report here that by means of concatenation of B10, we identified a quadruple concatemer 4B10 that displayed a markedly increased preS1-binding activity. The main binding site of 4B10 in preS1 was mapped to the receptor binding enhancing region. 4B10 blocked HBV attachment to hepatic cells and inhibited HBV infection of primary human and tupaia hepatocytes at low nanomolar concentrations. The 4B10-mediated inhibition of HBV infection is specific as it did not inhibit the infection of vesicular stomatitis virus glycoprotein pseudotyped lentivirus or human immunodeficiency virus type 1. Moreover, 4B10 showed no binding activity to hepatic cells. In conclusion, we have identified 4B10 as a promising candidate for a novel class of HBV entry inhibitors.

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