Yellow fever 17D-vectored vaccines expressing Lassa virus GP1 and GP2 glycoproteins provide protection against fatal disease in guinea pigs

Jiang, Xiaohong; Dalebout, Tim J.; Bredenbeek, Peter J.; Carrión, Ricardo; Brasky, Kathleen M.; Patterson, Jean L.; Goicochea, Marco; Bryant, Joseph; Salvato, María S.; Lukashevich, Igor S.

doi:10.1016/j.vaccine.2010.11.079

Cited by 74 publications

(60 citation statements)

References 56 publications

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“…The same electroporation device was also successfully used in HIV-1 DNA vaccine human trials (Kopycinski et al, 2012;Vasan et al, 2011). Since previous studies (Bredenbeek et al, 2006;Guy et al, 2010;Jiang et al, 2011) with recombinant YFV-17D-based vaccines showed that anti-vector immunity was a minor concern during prime-boost immunization, a prime-boost vaccination regimen was adopted to further augment the immune responses. Nevertheless, in vivo delivery of YFV infectious DNA by electroporation failed to induce YFVneutralizing antibodies in HLA-A2.1 transgenic C57BL/6 mice, despite readily detectable CD8 + T-cell responses, whereas YFV-17D vaccination of BALB/c mice was reported to yield a balanced Th1-Th2 immune response (Franco et al, 2010).…”

Section: Dna-launched Yfv-17dmentioning

confidence: 99%

“…YFV-17D has also been successfully exploited as a vector for the expression of foreign T-cell or B-cell epitopes, as potential vaccine candidates against malaria (Bonaldo et al, 2002;Tao et al, 2005) or as therapeutic anticancer vaccine (McAllister et al, 2000). Moreover, recombinant YFV-17D viruses expressing heterologous antigens were proposed as bivalent vaccine candidates against Lassa virus (Bredenbeek et al, 2006;Jiang et al, 2011) or as alternative vaccine vectors for malaria (Stoyanov et al, 2010) and HIV (Franco et al, 2010;Van Epps, 2005). In vitro characterization demonstrated that these recombinant viruses were viable and could express both YFV and foreign proteins.…”

Section: Introductionmentioning

confidence: 99%

“…Experiments in smallanimal models showed promising results in terms of immunogenicity and protection. Despite these encouraging results, genetic instability has been encountered for these recombinant viruses, especially with larger inserts, which is attributed to the limited packaging capacity of the icosahedral virion (Bonaldo et al, 2007;Jiang et al, 2011;Stoyanov et al, 2010).…”

Section: Introductionmentioning

confidence: 99%

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Molecular and immunological characterization of a DNA-launched yellow fever virus 17D infectious clone

Jiang

Dalebout

Lukashevich

et al. 2015

Journal of General Virology

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Yellow fever virus (YFV)-17D is an empirically developed, highly effective live-attenuated vaccine that has been administered to human beings for almost a century. YFV-17D has stood as a paradigm for a successful viral vaccine, and has been exploited as a potential virus vector for the development of recombinant vaccines against other diseases. In this study, a DNA-launched YFV-17D construct (pBeloBAC-FLYF) was explored as a new modality to the standard vaccine to combine the commendable features of both DNA vaccine and live-attenuated viral vaccine. The DNA-launched YFV-17D construct was characterized extensively both in cell culture and in mice. High titres of YFV-17D were generated upon transfection of the DNA into cells, whereas a mutant with deletion in the capsid-coding region (pBeloBAC-YF/DC) was restricted to a single round of infection, with no release of progeny virus. Homologous prime-boost immunization of AAD mice with both pBeloBAC-FLYF and pBeloBAC-YF/DC elicited specific dose-dependent cellular immune response against YFV-17D. Vaccination of A129 mice with pBeloBAC-FLYF resulted in the induction of YFV-specific neutralizing antibodies in all vaccinated subjects. These promising results underlined the potential of the DNA-launched YFV both as an alternative to standard YFV-17D vaccination and as a vaccine platform for the development of DNA-based recombinant YFV vaccines.

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Section: Dna-launched Yfv-17dmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Molecular and immunological characterization of a DNA-launched yellow fever virus 17D infectious clone

Jiang

Dalebout

Lukashevich

et al. 2015

Journal of General Virology

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show abstract

“…56,65,66 A similar approach was employed to improve the genetic stability of Lassa virus glycoproteins expressed by recombinant YF17D viruses in this genomic site. 67,68 Interestingly, a variant of this general methodology was described in the expression of the HIV clade B consensus Gag p24 sequence by the YF17D virus. In this case, the heterologous protein was directly expressed in frame with the YF E protein and fused to the single transmembrane anchoring segment of the Sindbis virus E2 protein.…”

Section: Expression Of Larger Fragments By the Yf17d Virusmentioning

confidence: 99%

“…Other studies confirmed the capacity of this YF E/NS1 viral platform to elicit a T cell-specific response against other antigens. 31,56,67,68,74,75 These results point to a need of optimization of vaccination regimens as well as an improvement of the YF E/ NS1 insertion platform immunogenicity, which should be considered since the yellow fever vaccine displays outstanding immunological properties as a human immunogen. Another possibility to exploit the expression of foreign proteins by the live-attenuated YF17D virus consists of the insertion of sequences into the C gene.…”

Section: Expression Of Larger Fragments By the Yf17d Virusmentioning

confidence: 99%