Literature DB >> 25793314

Structural basis for the neutralization of hepatitis E virus by a cross-genotype antibody.

Ying Gu1, Xuhua Tang2, Xiao Zhang3, Cuiling Song4, Minghua Zheng4, Kaihang Wang4, Jun Zhang3, Mun-Hon Ng1, Choy-Leong Hew5, Shaowei Li1, Ningshao Xia1, J Sivaraman6.   

Abstract

Hepatitis E virus (HEV), a non-enveloped, positive-sense, single-stranded RNA virus, is a major cause of enteric hepatitis. Classified into the family Hepeviridae, HEV comprises four genotypes (genotypes 1-4), which belong to a single serotype. We describe a monoclonal antibody (mAb), 8G12, which equally recognizes all four genotypes of HEV, with ∼ 2.53-3.45 nM binding affinity. The mAb 8G12 has a protective, neutralizing capacity, which can significantly block virus infection in host cells. Animal studies with genotypes 1, 3 and 4 confirmed the cross-genotype neutralizing capacity of 8G12 and its effective prevention of hepatitis E disease. The complex crystal structures of 8G12 with the HEV E2s domain (the most protruded region of the virus capsid) of the abundant genotypes 1 and 4 were determined at 4.0 and 2.3 Å resolution, respectively. These structures revealed that 8G12 recognizes both genotypes through the epitopes in the E2s dimerization region. Structure-based mutagenesis and cell-model assays with virus-like particles identified several conserved residues (Glu549, Lys554 and Gly591) that are essential for 8G12 neutralization. Moreover, the epitope of 8G12 is identified as a key epitope involved in virus-host interactions. These findings will help develop a common strategy for the prevention of the most abundant form of HEV infection.

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Year:  2015        PMID: 25793314      PMCID: PMC4423075          DOI: 10.1038/cr.2015.34

Source DB:  PubMed          Journal:  Cell Res        ISSN: 1001-0602            Impact factor:   25.617


  38 in total

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3.  Likelihood-enhanced fast rotation functions.

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4.  Crystallography & NMR system: A new software suite for macromolecular structure determination.

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Journal:  Acta Crystallogr D Biol Crystallogr       Date:  1998-09-01

5.  Amino-terminal epitopes are exposed when full-length open reading frame 2 of hepatitis E virus is expressed in Escherichia coli, but carboxy-terminal epitopes are masked.

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6.  Evaluation of antibody-based and nucleic acid-based assays for diagnosis of hepatitis E virus infection in a rhesus monkey model.

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Journal:  J Med Virol       Date:  2003-12       Impact factor: 2.327

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Authors:  S P Jaiswal; A K Jain; G Naik; N Soni; D S Chitnis
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8.  PreS1-specific binding proteins as potential receptors for hepatitis B virus in human hepatocytes.

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Authors:  A W Tam; M M Smith; M E Guerra; C C Huang; D W Bradley; K E Fry; G R Reyes
Journal:  Virology       Date:  1991-11       Impact factor: 3.616

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  28 in total

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2.  Establishment of a Highly Sensitive Assay for Detection of Hepatitis E Virus-Specific Immunoglobulins.

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3.  Dynamics of 8G12 competitive antibody in "prime-boost" vaccination of Hepatitis E vaccine.

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4.  Effect of freezing on recombinant hepatitis E vaccine.

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6.  Functional epitopes on hepatitis E virions and recombinant capsids are highly conformation-dependent.

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7.  Origin, antigenicity, and function of a secreted form of ORF2 in hepatitis E virus infection.

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8.  Characterization of Three Novel Linear Neutralizing B-Cell Epitopes in the Capsid Protein of Swine Hepatitis E Virus.

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9.  Phage-displayed peptides that mimic epitopes of hepatitis E virus capsid.

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Review 10.  Hepatitis E virus: Current epidemiology and vaccine.

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