Literature DB >> 10644345

Chimeric yellow fever virus 17D-Japanese encephalitis virus vaccine: dose-response effectiveness and extended safety testing in rhesus monkeys.

T P Monath1, I Levenbook, K Soike, Z X Zhang, M Ratterree, K Draper, A D Barrett, R Nichols, R Weltzin, J Arroyo, F Guirakhoo.   

Abstract

ChimeriVax-JE is a live, attenuated recombinant virus prepared by replacing the genes encoding two structural proteins (prM and E) of yellow fever 17D virus with the corresponding genes of an attenuated strain of Japanese encephalitis virus (JE), SA14-14-2 (T. J. Chambers et al., J. Virol. 73:3095-3101, 1999). Since the prM and E proteins contain antigens conferring protective humoral and cellular immunity, the immune response to vaccination is directed principally at JE. The prM-E genome sequence of the ChimeriVax-JE in diploid fetal rhesus lung cells (FRhL, a substrate acceptable for human vaccines) was identical to that of JE SA14-14-2 vaccine and differed from sequences of virulent wild-type strains (SA14 and Nakayama) at six amino acid residues in the envelope gene (E107, E138, E176, E279, E315, and E439). ChimeriVax-JE was fully attenuated for weaned mice inoculated by the intracerebral (i.c.) route, whereas commercial yellow fever 17D vaccine (YF-Vax) caused lethal encephalitis with a 50% lethal dose of 1.67 log(10) PFU. Groups of four rhesus monkeys were inoculated by the subcutaneous route with 2.0, 3.0, 4.0, and 5. 0 log(10) PFU of ChimeriVax-JE. All 16 monkeys developed low viremias (mean peak viremia, 1.7 to 2.1 log(10) PFU/ml; mean duration, 1.8 to 2.3 days). Neutralizing antibodies appeared between days 6 and 10; by day 30, neutralizing antibody responses were similar across dose groups. Neutralizing antibody titers to the homologous (vaccine) strain were higher than to the heterologous wild-type JE strains. All immunized monkeys and sham-immunized controls were challenged i.c. on day 54 with 5.2 log(10) PFU of wild-type JE. None of the immunized monkeys developed viremia or illness and had mild residual brain lesions, whereas controls developed viremia, clinical encephalitis, and severe histopathologic lesions. Immunized monkeys developed significant (>/=4-fold) increases in serum and cerebrospinal fluid neutralizing antibodies after i.c. challenge. In a standardized test for neurovirulence, ChimeriVax-JE and YF-Vax were compared in groups of 10 monkeys inoculated i.c. and analyzed histopathologically on day 30. Lesion scores in brains and spinal cord were significantly higher for monkeys inoculated with YF-Vax. ChimeriVax-JE meets preclinical safety and efficacy requirements for a human vaccine; it appears safer than yellow fever 17D vaccine but has a similar profile of immunogenicity and protective efficacy.

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Year:  2000        PMID: 10644345      PMCID: PMC111650          DOI: 10.1128/jvi.74.4.1742-1751.2000

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


  30 in total

1.  The anamnestic antibody response to Japanese encephalitis virus in monkeys and its implications concerning naturally acquired immunity in man.

Authors:  H W LEE; W F SCHERER
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2.  Recombinant, chimaeric live, attenuated vaccine (ChimeriVax) incorporating the envelope genes of Japanese encephalitis (SA14-14-2) virus and the capsid and nonstructural genes of yellow fever (17D) virus is safe, immunogenic and protective in non-human primates.

Authors:  T P Monath; K Soike; I Levenbook; Z X Zhang; J Arroyo; S Delagrave; G Myers; A D Barrett; R E Shope; M Ratterree; T J Chambers; F Guirakhoo
Journal:  Vaccine       Date:  1999-04-09       Impact factor: 3.641

3.  The envelope glycoprotein from tick-borne encephalitis virus at 2 A resolution.

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4.  Molecular basis of attenuation of neurovirulence of wild-type Japanese encephalitis virus strain SA14.

Authors:  H Ni; G J Chang; H Xie; D W Trent; A D Barrett
Journal:  J Gen Virol       Date:  1995-02       Impact factor: 3.891

5.  Protection against Japanese encephalitis by inactivated vaccines.

Authors:  C H Hoke; A Nisalak; N Sangawhipa; S Jatanasen; T Laorakapongse; B L Innis; S Kotchasenee; J B Gingrich; J Latendresse; K Fukai
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Authors:  T J Chambers; A Nestorowicz; P W Mason; C M Rice
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7.  Genetic variation of Japanese encephalitis virus in nature.

Authors:  W R Chen; R B Tesh; R Rico-Hesse
Journal:  J Gen Virol       Date:  1990-12       Impact factor: 3.891

8.  An intranasal challenge model for testing Japanese encephalitis vaccines in rhesus monkeys.

Authors:  B Raengsakulrach; A Nisalak; M Gettayacamin; V Thirawuth; G D Young; K S Myint; L M Ferguson; C H Hoke; B L Innis; D W Vaughn
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9.  Antigenic characterization of the live attenuated Japanese encephalitis vaccine virus SA14-14-2: a comparison with isolates of the virus covering a wide geographic area.

Authors:  M R Wills; B K Sil; J X Cao; Y X Yu; A D Barrett
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10.  Identification of mutations that occurred on the genome of Japanese encephalitis virus during the attenuation process.

Authors:  S Aihara; C M Rao; Y X Yu; T Lee; K Watanabe; T Komiya; H Sumiyoshi; H Hashimoto; A Nomoto
Journal:  Virus Genes       Date:  1991-04       Impact factor: 2.332

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2.  Attenuation of Murray Valley encephalitis virus by site-directed mutagenesis of the hinge and putative receptor-binding regions of the envelope protein.

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3.  Sequential immunization with heterologous chimeric flaviviruses induces broad-spectrum cross-reactive CD8+ T cell responses.

Authors:  Rekha Singh; Alan L Rothman; James Potts; Farshad Guirakhoo; Francis A Ennis; Sharone Green
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7.  Attenuation of recombinant yellow fever 17D viruses expressing foreign protein epitopes at the surface.

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8.  Neuropathogenesis and neurovirulence of live flaviviral vaccines in monkeys.

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9.  A single amino acid substitution in the envelope protein of chimeric yellow fever-dengue 1 vaccine virus reduces neurovirulence for suckling mice and viremia/viscerotropism for monkeys.

Authors:  F Guirakhoo; Z Zhang; G Myers; B W Johnson; K Pugachev; R Nichols; N Brown; I Levenbook; K Draper; S Cyrek; J Lang; C Fournier; B Barrere; S Delagrave; T P Monath
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10.  Safety and efficacy of chimeric yellow Fever-dengue virus tetravalent vaccine formulations in nonhuman primates.

Authors:  F Guirakhoo; K Pugachev; Z Zhang; G Myers; I Levenbook; K Draper; J Lang; S Ocran; F Mitchell; M Parsons; N Brown; S Brandler; C Fournier; B Barrere; F Rizvi; A Travassos; R Nichols; D Trent; T Monath
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