2018
DOI: 10.1016/j.vaccine.2018.07.056
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Novel trimeric human cytomegalovirus glycoprotein B elicits a high-titer neutralizing antibody response

Abstract: Human cytomegalovirus (HCMV) is a major cause of disability in congenitally infected infants and in the immunosuppressed. There is currently no licensed prophylactic HCMV vaccine. The HCMV envelope glycoprotein B (gB) is considered a major vaccine target antigen based on its critical role in mediating viral-host cell fusion and thus viral entry. The natural conformation of HCMV gB within the viral envelope is a trimer, but there has been no reported success in producing a recombinant trimeric gB suitable for v… Show more

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Cited by 35 publications
(53 citation statements)
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“…We have produced, within CHO cells, a trimeric HCMV gB by insertion of a flexible 15 amino acid (Gly 4 Ser) 3 linker at the furin cleavage site that allowed for terminal protein folding and efficient expression. 53 Trimeric HCMV gB induced 5to 11-fold higher serum titers of gB-specific IgG relative to monomeric HCMV gB similar to the Chiron gB that was previously used in phase II clinical trials and elicited 50-fold higher complement-independent HCMV neutralization activity, suggesting that conformational epitopes of the trimeric HCMV gB played an important role in eliciting neutralization activity. 53 Soluble monomeric HCMV gB as well as different post-fusion HCMV trimeric gBs elicited mainly complementdependent HCMV-neutralizing antibodies.…”
Section: Novatis Modernamentioning
confidence: 84%
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“…We have produced, within CHO cells, a trimeric HCMV gB by insertion of a flexible 15 amino acid (Gly 4 Ser) 3 linker at the furin cleavage site that allowed for terminal protein folding and efficient expression. 53 Trimeric HCMV gB induced 5to 11-fold higher serum titers of gB-specific IgG relative to monomeric HCMV gB similar to the Chiron gB that was previously used in phase II clinical trials and elicited 50-fold higher complement-independent HCMV neutralization activity, suggesting that conformational epitopes of the trimeric HCMV gB played an important role in eliciting neutralization activity. 53 Soluble monomeric HCMV gB as well as different post-fusion HCMV trimeric gBs elicited mainly complementdependent HCMV-neutralizing antibodies.…”
Section: Novatis Modernamentioning
confidence: 84%
“…53 Trimeric HCMV gB induced 5to 11-fold higher serum titers of gB-specific IgG relative to monomeric HCMV gB similar to the Chiron gB that was previously used in phase II clinical trials and elicited 50-fold higher complement-independent HCMV neutralization activity, suggesting that conformational epitopes of the trimeric HCMV gB played an important role in eliciting neutralization activity. 53 Soluble monomeric HCMV gB as well as different post-fusion HCMV trimeric gBs elicited mainly complementdependent HCMV-neutralizing antibodies. [79][80][81] In contrast, the trimeric HCMV gB produced in our laboratory elicited markedly higher serum HCMV-neutralizing antibodies that exhibited both complement-independent and complementdependent activity.…”
Section: Novatis Modernamentioning
confidence: 84%
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