A Subunit Cytomegalovirus Vaccine Based on Recombinant Envelope Glycoprotein B and a New Adjuvant

Pass, Robert F.; Duliegè, Anne-Marie; Boppana, Suresh B.; Sekulovich, Rose E.; Percell, Sandra; Britt, William J.; Burke, Rae Lyn

doi:10.1086/315022

Cited by 227 publications

(135 citation statements)

References 18 publications

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“…51 Subunit vaccines incorporating only pp65, IE-1, and gB have been developed and elicit both T-cell and antibody responses. 52,53 Studies to identify the viral genes that encode additional CMV antigens recognized by CD8 ϩ CTLs and to elucidate their role in protective immunity should provide insights into the necessity to incorporate additional determinants in a CMV vaccine. …”

Section: Discussionmentioning

confidence: 99%

Immune evasion proteins of human cytomegalovirus do not prevent a diverse CD8+ cytotoxic T-cell response in natural infection

Manley

Luy

Jones

et al. 2004

Blood

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Although cytomegalovirus (CMV) expresses proteins that interfere with antigen presentation by class I major histocompatibility complex (MHC) molecules, CD8 ؉ cytotoxic T cells (CTLs) are indispensable for controlling infection and maintaining latency. Here, a cytokine flow cytometry assay that employs fibroblasts infected with a mutant strain of CMV (RV798), which is deleted of the 4 viral genes that are responsible for interfering with class I MHC presentation, was used to examine the frequency and specificity of the CD8 ؉ CTLs to CMV in immunocompetent CMV-seropositive individuals. A large fraction of the CD8 ؉ CTL response was found to be specific for viral antigens expressed during the immediate early and early phases of virus replication and presented by fibroblasts infected with RV798 but not wild-type CMV. These results demonstrate that the inhibition of class I antigen presentation observed in CMV-infected cells in vitro is not sufficient to prevent the induction of a broad repertoire of CD8 ؉ CTLs after natural infection in vivo. Thus, reconstitution of T-cell immunity in immunodeficient patients by cell therapy or by vaccination may need to target multiple viral antigens to completely restore immunologic control of

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Section: Discussionmentioning

confidence: 99%

Immune evasion proteins of human cytomegalovirus do not prevent a diverse CD8+ cytotoxic T-cell response in natural infection

Manley

Luy

Jones

et al. 2004

Blood

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show abstract

“…Although a larger numbers of Mmu are needed to conWrm this observation, it further indicates the protective role of neutralizing antibodies against CMV [14,17,18,24] and a gB-based vaccine strategy [15,17,25]. Natural immunity studies have suggested that a vaccine that stimulates immunity equivalent to levels associated with natural infection could reduce the morbidity due to congenital CMV infection by »80% [8,9].…”

Section: #6 Controlmentioning

confidence: 93%

Evaluation of recombinant modified vaccinia Ankara virus-based rhesus cytomegalovirus vaccines in rhesus macaques

Yue

Wang

Abel

et al. 2008

Med Microbiol Immunol

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A vaccine consisting of rhesus cytomegalovirus (RhCMV) pp65-2, gB and IE1 expressed via modiWed vaccinia Ankara (MVA) was evaluated in rhesus macaques with or without prior priming with expression plasmids for the same antigens. Following two MVA treatments, comparable levels of anti-gB, pp65-2 and neutralizing antibody responses, and pp65-2-and IE1-speciWc cellular immune responses were detected in both vaccinated groups. Similar reductions in plasma peak viral loads were observed in these groups compared to untreated controls. This study demonstrates the immunogenicity and protective eYcacy of rMVA-based RhCMV subunit vaccines in a primate host and warrants further investigation to improve the eYcacy of subunit vaccines against CMV.

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“…Preliminary results from human Phase I trials of recombinant gB vaccine suggest that the vaccine is safe and immunogenic. [47][48][49] While promising, these vaccines have yet to proceed past initial safety trials.…”

mentioning

confidence: 99%

A DNA-Based Vaccine for the Prevention of Human Cytomegalovirus-Associated Diseases

Selinsky

Luke²,

Wloch³

et al. 2005

Human Vaccines

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A Subunit Cytomegalovirus Vaccine Based on Recombinant Envelope Glycoprotein B and a New Adjuvant

Cited by 227 publications

References 18 publications

Immune evasion proteins of human cytomegalovirus do not prevent a diverse CD8+ cytotoxic T-cell response in natural infection

Immune evasion proteins of human cytomegalovirus do not prevent a diverse CD8+ cytotoxic T-cell response in natural infection

Evaluation of recombinant modified vaccinia Ankara virus-based rhesus cytomegalovirus vaccines in rhesus macaques

A DNA-Based Vaccine for the Prevention of Human Cytomegalovirus-Associated Diseases

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