A Spread-Deficient Cytomegalovirus for Assessment of First-Target Cells in Vaccination

Mohr, Hermine; Arapović, Jurica; Mühlbach, Hermine; Panzer, Marc; Weyn, Annelies; Dölken, Lars; Krmpotić, Astrid; Voehringer, David; Ruzsics, Zsolt; Koszinowski, Ulrich H.; Sacher, Torsten

doi:10.1128/jvi.02696-09

Cited by 43 publications

(59 citation statements)

References 80 publications

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“…The vaccination potential of CMV mutants lacking nonessential viral genes has already been proven (33,34). Also, spread-deficient MCMV lacking the essential gene M94 induced a virus-specific immune response and proved to be safe in an immunodeficient host (31). The approach of the present study was to generate an experimental vaccine expressing NKG2D ligand, which is therefore attenuated due to strong immune control and, at the same time, resistant to viral immunoevasion of this signaling pathway.…”

Section: Discussionmentioning

confidence: 99%

“…Still, a live, attenuated vaccine approach has several characteristics that render it attractive. Unlike subunit vaccines, which induce cellular or humoral immune response to selected antigens only, live vaccines induce a much broader immunity that may mimic protection acquired following natural infection (31,33,(66)(67)(68)(69). Cellular immunity against CMV follows unique kinetics characterized by maintenance or even expansion of the virus-specific CD8 + T cell response over time (70,71).…”

Section: Discussionmentioning

confidence: 99%

“…A number of subunit vaccine strategies and live, attenuated CMV vaccines have been developed (27)(28)(29)(30)(31). Recently, a phase II clinical trial was described that suggested a protective capacity against maternal infection by use of recombinant monovalent gB HCMV vaccine (32).…”

Section: Introductionmentioning

confidence: 99%

“…Their use, however, carries the risk of CMV disease caused by the vaccine strain or reactivation in the immunocompromised state, unless the vaccine virus is efficiently controlled by residual immunity. One approach to generating such an immunogenic, yet safe live vaccine is deletion of viral genes that subvert the host immune response (33,34) or essential genes resulting in spread-deficient virus (31). The other approach is the insertion of a ligand recognized by the activating receptor on immune cells into the CMV genome.…”

Section: Introductionmentioning

confidence: 99%

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Recombinant mouse cytomegalovirus expressing a ligand for the NKG2D receptor is attenuated and has improved vaccine properties

Slavuljica¹,

Busche²,

Babić³

et al. 2010

J. Clin. Invest.

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105

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Human CMV (HCMV) is a major cause of morbidity and mortality in both congenitally infected and immunocompromised individuals. Development of an effective HCMV vaccine would help protect these vulnerable groups. NK group 2, member D (NKG2D) is a potent activating receptor expressed by cells of the innate and adaptive immune systems. Its importance in HCMV immune surveillance is indicated by the elaborative evasion mechanisms evolved by the virus to avoid NKG2D. In order to study this signaling pathway, we engineered a recombinant mouse CMV expressing the high-affinity NKG2D ligand RAE-1γ (RAE-1γMCMV). Expression of RAE-1γ by MCMV resulted in profound virus attenuation in vivo and lower latent viral DNA loads. RAE-1γMCMV infection was efficiently controlled by immunodeficient hosts, including mice lacking type I interferon receptors or immunosuppressed by sublethal γ-irradiation. Features of MCMV infection in neonates were also diminished. Despite tight innate immune control, RAE-1γMCMV infection elicited strong and long-lasting protective immunity. Maternal RAE-1γMCMV immunization protected neonatal mice from MCMV disease via placental transfer of antiviral Abs. Despite strong selective pressure, the RAE-1γ transgene did not exhibit sequence variation following infection. Together, our results indicate that use of a recombinant virus encoding the ligand for an activating NK cell receptor could be a powerful approach to developing a safe and immunogenic HCMV vaccine.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Recombinant mouse cytomegalovirus expressing a ligand for the NKG2D receptor is attenuated and has improved vaccine properties

Slavuljica¹,

Busche²,

Babić³

et al. 2010

J. Clin. Invest.

Self Cite

105

View full text Add to dashboard Cite

show abstract

“…Since primary infection with RhCMV 68-1 (the parental strain of ΔUS2-11gag) does not result in robust viremia (see below), direct measurements of viral loads were unlikely to be informative. Instead, we used the development of anti-CMV antibodies as a surrogate for CMV antigen load, because it was shown previously in the murine model that reduced viral spread correlates with reduced antibody responses but does not affect T cell responses (47). However, when lysates Genome copy numbers in tissue samples are given per 10 7 cell equivalents, whereas genome copies in urine and plasma are shown per ml.…”

Section: Vaccine-induced Pp65-specific T Cells Do Not Recapitulate Thmentioning

confidence: 99%

Cytomegalovirus pp65 limits dissemination but is dispensable for persistence

et al. 2014

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The most abundantly produced virion protein in human cytomegalovirus (HCMV) is the immunodominant phosphoprotein 65 (pp65), which is frequently included in CMV vaccines. Although it is nonessential for in vitro CMV growth, pp65 displays immunomodulatory functions that support a potential role in primary and/or persistent infection. To determine the contribution of pp65 to CMV infection and immunity, we generated a rhesus CMV lacking both pp65 orthologs (RhCMVΔpp65ab). While deletion of pp65ab slightly reduced growth in vitro and increased defective particle formation, the protein composition of secreted virions was largely unchanged. Interestingly, pp65 was not required for primary and persistent infection in animals. Immune responses induced by RhCMVΔpp65ab did not prevent reinfection with rhesus CMV; however, reinfection with RhCMVΔUS2-11, which lacks viral-encoded MHC-I antigen presentation inhibitors, was prevented. Unexpectedly, induction of pp65b-specific T cells alone did not protect against RhCMVΔUS2-11 challenge, suggesting that T cells targeting multiple CMV antigens are required for protection. However, pp65-specific immunity was crucial for controlling viral dissemination during primary infection, as indicated by the marked increase of RhCMVΔpp65ab genome copies in CMV-naive, but not CMV-immune, animals. Our data provide rationale for inclusion of pp65 into CMV vaccines but also demonstrate that pp65-induced T cell responses alone do not recapitulate the protective effect of natural infection.

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Recent Approaches and Strategies in the Generation of Anti-human Cytomegalovirus Vaccines

Boppana

Britt

2021

Methods in Molecular Biology

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A Spread-Deficient Cytomegalovirus for Assessment of First-Target Cells in Vaccination

Cited by 43 publications

References 80 publications

Recombinant mouse cytomegalovirus expressing a ligand for the NKG2D receptor is attenuated and has improved vaccine properties

Recombinant mouse cytomegalovirus expressing a ligand for the NKG2D receptor is attenuated and has improved vaccine properties

Cytomegalovirus pp65 limits dissemination but is dispensable for persistence

Recent Approaches and Strategies in the Generation of Anti-human Cytomegalovirus Vaccines

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