Literature DB >> 21177825

Hepatitis B virus surface antigen assembly function persists when entire transmembrane domains 1 and 3 are replaced by a heterologous transmembrane sequence.

Ira Berkower1, Angelo Spadaccini, Hong Chen, Danah Al-Awadi, Jacqueline Muller, Yamei Gao, Dino Feigelstock, Konstantin Virnik, Yisheng Ni.   

Abstract

Native hepatitis B surface antigen (HBsAg) spontaneously assembles into 22-nm subviral particles. The particles are lipoprotein micelles, in which HBsAg is believed to span the lipid layer four times. The first two transmembrane domains, TM1 and TM2, are required for particle assembly. We have probed the requirements for particle assembly by replacing the entire first or third TM domain of HBsAg with the transmembrane domain of HIV gp41. We found that either TM domain of HBsAg could be replaced, resulting in HBsAg-gp41 chimeras that formed particles efficiently. HBsAg formed particles even when both TM1 and TM3 were replaced with the gp41 domain. The results indicate remarkable flexibility in HBsAg particle formation and provide a novel way to express heterologous membrane proteins that are anchored to a lipid surface by their own membrane-spanning domain. The membrane-proximal exposed region (MPER) of gp41 is an important target of broadly reactive neutralizing antibodies against HIV-1, and HBsAg-MPER particles may provide a good platform for future vaccine development.

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Year:  2010        PMID: 21177825      PMCID: PMC3067800          DOI: 10.1128/JVI.02061-10

Source DB:  PubMed          Journal:  J Virol        ISSN: 0022-538X            Impact factor:   5.103


  48 in total

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4.  Analysis of the human immunodeficiency virus type 1 gp41 membrane proximal external region arrayed on hepatitis B surface antigen particles.

Authors:  S Phogat; K Svehla; M Tang; A Spadaccini; J Muller; J Mascola; I Berkower; R Wyatt
Journal:  Virology       Date:  2007-12-26       Impact factor: 3.616

5.  Chimeric hepatitis B and C viruses envelope proteins can form subviral particles: implications for the design of new vaccine strategies.

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6.  A topological model for hepatitis B surface antigen.

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7.  Expression and characterization of hepatitis B virus surface antigen polypeptides in insect cells with a baculovirus expression system.

Authors:  R E Lanford; V Luckow; R C Kennedy; G R Dreesman; L Notvall; M D Summers
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8.  Establishment of retroviral pseudotypes with influenza hemagglutinins from H1, H3, and H5 subtypes for sensitive and specific detection of neutralizing antibodies.

Authors:  Wei Wang; Eboneé N Butler; Vic Veguilla; Russell Vassell; J Terrig Thomas; Malcolm Moos; Zhiping Ye; Kathy Hancock; Carol D Weiss
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9.  The first transmembrane domain of the hepatitis B virus large envelope protein is crucial for infectivity.

Authors:  Charlotte Lepère-Douard; Maud Trotard; Jacques Le Seyec; Philippe Gripon
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10.  The role of envelope proteins in hepatitis B virus assembly.

Authors:  V Bruss; D Ganem
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6.  3D visualisation of hepatitis B vaccine in the oral delivery vehicle SBA-15.

Authors:  Martin K Rasmussen; Nikolay Kardjilov; Cristiano L P Oliveira; Benjamin Watts; Julie Villanova; Viviane Fongaro Botosso; Osvaldo A Sant'Anna; Marcia C A Fantini; Heloisa N Bordallo
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Review 7.  Extracellular RNA in viral-host interactions: Thinking outside the cell.

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8.  Occult HBV infection in Chinese blood donors: role of N-glycosylation mutations and amino acid substitutions in S protein transmembrane domains.

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  8 in total

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