Studies of AIDS vaccination using an ex vivo feline immunodeficiency virus model: protection conferred by a fixed-cell vaccine against cell-free and cell-associated challenge differs in duration and is not easily boosted

Matteucci, Donatella; Pistello, Mauro; Mazzetti, Paola; Giannecchini, Simone; Mauro, Daniela; Lonetti, Isabella; Zaccaro, Lucia; Pollera, C.; Specter, Steven; Bendinelli, Mauro

doi:10.1128/jvi.71.11.8368-8376.1997

Cited by 30 publications

(24 citation statements)

References 46 publications

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“…When placed in a free-roaming shelter for 22 months with natural FIV-infected cats, this single-subtype vaccine protected the vaccinated group of cats (0/12 FIV infection rate) whereas 5/14 of the unvaccinated control group became infected . A major limitation of inactivated infected-cell vaccines is the short duration of vaccine immunity compared to inactivated whole virus vaccines (Matteucci et al, 1997;Tellier et al, 1998). Since the level of the FIV exposure during natural transmission remains unknown, the ef®cacy evaluation using a contact challenge system represents the ultimate test for any commercial FIV vaccine.…”

Section: Fiv Vaccine Studiesmentioning

confidence: 99%

“…Among these FIV vaccine designs, VN antibody induction was more consistent in cats immunized with conventional inactivated virus vaccine followed by recombinant vectored vaccine (Tellier et al, 1998;Giannecchini et al, 2001;Pu et al, 2001). Although, inactivated infectedcell vaccine may induce higher VN antibody levels compared to inactivated whole virus vaccine, the duration of protection may be shorter in the inactivated infected-cell vaccine group (Matteucci et al, 1997). Unlike human AIDS research which test HIV vaccine antibodies for their ability to neutralize both labora-tory and clinical isolates, FIV vaccine researchers have not tested their vaccine antibodies against nonadapted clinical isolates (Matteucci et al, 1997;Pu et al, 2001).…”

Section: Immune Correlate Of Vaccine Protectionmentioning

confidence: 99%

“…Although, inactivated infectedcell vaccine may induce higher VN antibody levels compared to inactivated whole virus vaccine, the duration of protection may be shorter in the inactivated infected-cell vaccine group (Matteucci et al, 1997). Unlike human AIDS research which test HIV vaccine antibodies for their ability to neutralize both labora-tory and clinical isolates, FIV vaccine researchers have not tested their vaccine antibodies against nonadapted clinical isolates (Matteucci et al, 1997;Pu et al, 2001). FIV laboratories now test the crossneutralizing ability of sera from naturally and experimentally infected cats against clinical and laboratory isolates (Inoshima et al, 1998;Pu et al, 2001).…”

Section: Immune Correlate Of Vaccine Protectionmentioning

confidence: 99%

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FIV vaccine development and its importance to veterinary and human medicine: a review

Uhl

Heaton-Jones

et al. 2002

Veterinary Immunology and Immunopathology

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Feline immunodeficiency virus (FIV) is a natural infection of domestic cats that results in acquired immunodeficiency syndrome resembling human immunodeficiency virus (HIV) infection in humans. The worldwide prevalence of FIV infection in domestic cats has been reported to range from 1 to 28%. Hence, an effective FIV vaccine will have an important impact on veterinary medicine in addition to being used as a small animal AIDS model for humans. Since the discovery of FIV reported in 1987, FIV vaccine research has pursued both molecular and conventional vaccine approaches toward the development of a commercial product. Published FIV vaccine trial results from 1998 to the present have been compiled to update the veterinary clinical and research communities on the immunologic and experimental efficacy status of these vaccines. A brief report is included on the outcome of the 10 years of collaborative work between industry and academia which led to recent USDA approval of the first animal lentivirus vaccine, the dual-subtype FIV vaccine. The immunogenicity and efficacy of the experimental prototype, dual-subtype FIV vaccine and the efficacy of the currently approved commercial, dual-subtype FIV vaccine (Fel-O-Vax FIV) are discussed. Potential cross-reactivity complications between commercial FIV diagnostic tests, Idexx Snap Combo Test and Western blot assays, and sera from previously vaccinated cats are also discussed. Finally, recommendations are made for unbiased critical testing of new FIV vaccines, the currently USDA approved vaccine, and future vaccines in development.

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Section: Fiv Vaccine Studiesmentioning

confidence: 99%

Section: Immune Correlate Of Vaccine Protectionmentioning

confidence: 99%

Section: Immune Correlate Of Vaccine Protectionmentioning

confidence: 99%

See 1 more Smart Citation

FIV vaccine development and its importance to veterinary and human medicine: a review

Uhl

Heaton-Jones

et al. 2002

Veterinary Immunology and Immunopathology

View full text Add to dashboard Cite

show abstract

“…Confirmation of the efficacy of vaccines containing FIV-infected cells was provided by Matteucci et al 47 A vaccine based on paraformaldehydeinactivated cells of the MBM feline lymphoblast line infected with FIV-M2 protected cats when challenged with ex vivo, cell-free virus 4 months after vaccination. No significant protection was recorded when the cats were challenged 12 or 28 months after vaccination, indicating that the duration of immunity was short.…”

Section: Inactivated Virus-infected Cell Vaccinesmentioning

confidence: 94%

FIV as a Model for AIDS Vaccine Studies

Dunham

Jarrett

In Vivo Models of HIV Disease and Control

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“…528 Duration of WKV and FC vaccineinduced protection has been another concern, with some vaccine studies revealing a breakthrough in vaccine-induced protection a year after vaccination despite boostering the primary immunization. 529,530 Another concern relates to differences in WKV or FC vaccine-induced protection observed against similar challenge viruses but delivered by different routes of exposure, including parenteral and mucosal delivery. 526 Collectively these findings suggest that WKV vaccines demonstrate significant potential for development of lentivirus vaccines, but that multiple issues including WKV vaccine-induced enhancement still require attention for achievement of optimal protection.…”

Section: Fiv Wkv and Fixed-cell Vaccinesmentioning

confidence: 99%

FIV as a Model for HIV: An Overview

Sparger

In Vivo Models of HIV Disease and Control

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Studies of AIDS vaccination using an ex vivo feline immunodeficiency virus model: protection conferred by a fixed-cell vaccine against cell-free and cell-associated challenge differs in duration and is not easily boosted

Cited by 30 publications

References 46 publications

FIV vaccine development and its importance to veterinary and human medicine: a review

FIV vaccine development and its importance to veterinary and human medicine: a review

FIV as a Model for AIDS Vaccine Studies

FIV as a Model for HIV: An Overview

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