Efficacy of a canarypox-vectored recombinant vaccine expressing the hemagglutinin gene of equine influenza H3N8 virus in the protection of ponies from viral challenge

Minke, J.M.; Toulemonde, C. Edlund; Coupier, Hervé; Guigal, Pierre-Michel; Dinic, S.; Sindle, T.; Jessett, D.M.; Black, L; Bublot, Michel; Pardo, M.C.; Audonnet, Jean-Christophe

doi:10.2460/ajvr.68.2.213

Cited by 59 publications

(45 citation statements)

References 25 publications

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“…The canarypox virus vector is already used in several licensed commercial vaccines worldwide, including for horses (21), (24), (36) and (37). The ALVAC-EIV vaccine contains antigens for two strains of equine influenza virus (24) demonstrating that the ALVAC construct can be used successfully to vaccinate against multiple antigens simultaneously. This property of the construct needs to be further evaluated for the possible development of polyvalent AHSV vaccines.…”

Section: Discussionmentioning

confidence: 99%

“…For ethical reasons, only a single control horse was used to confirm the virulence of the challenge inoculum because this virus strain has previously been shown to cause severe or lethal disease in inoculated horses (19). The control horse was vaccinated with ALVAC-EIV expressing the haemagglutinin proteins of two equine influenza H3N8 viruses (PROTEQFLU, Merial) that was administered according to the manufacturer's instructions (24). All horses were revaccinated 28 days later with the respective vaccine construct.…”

Section: Vaccination Of Horses With Alvac-ahsvmentioning

confidence: 99%

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Protective immunization of horses with a recombinant canarypox virus vectored vaccine co-expressing genes encoding the outer capsid proteins of African horse sickness virus

Guthrie¹,

Quan²,

Lourens³

et al. 2009

Vaccine

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We describe the development and preliminary characterization of a recombinant canarypox virus vectored (ALVAC ® ) vaccine for protective immunization of equids against African horse sickness virus (AHSV) infection. Horses (n = 8) immunized with either of two concentrations of recombinant canarypox virus vector (ALVAC-AHSV) co-expressing synthetic genes encoding the outer capsid proteins (VP2 and VP5) of AHSV serotype 4 (AHSV-4) developed variable titres (<10-80) of virus-specific neutralizing antibodies and were completely resistant to challenge infection with a virulent strain of AHSV-4. In contrast, a horse immunized with a commercial recombinant canarypox virus vectored vaccine expressing the haemagglutinin genes of two equine influenza H3N8 viruses was seronegative to AHSV and following infection with virulent AHSV-4 developed pyrexia, thrombocytopenia and marked oedema of the supraorbital fossae typical of the "dikkop" or cardiac form of African horse sickness. AHSV was detected by virus isolation and quantitative reverse transcriptase polymerase chain reaction in the blood of the control horse from 8 days onwards after challenge infection whereas AHSV was not detected at any time in the blood of the ALVAC-AHSV vaccinated horses. The control horse seroconverted to AHSV by 2 weeks after challenge infection as determined by both virus neutralization and ELISA assays, whereas six of eight of the ALVAC-AHSV vaccinated horses did not seroconvert by either assay following challenge infection with virulent AHSV-4. These data confirm that the ALVAC-AHSV vaccine will be useful for the protective immunization of equids against African horse sickness, and avoids many of the problems inherent to liveattenuated AHSV vaccines.

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Section: Discussionmentioning

confidence: 99%

Section: Vaccination Of Horses With Alvac-ahsvmentioning

confidence: 99%

Protective immunization of horses with a recombinant canarypox virus vectored vaccine co-expressing genes encoding the outer capsid proteins of African horse sickness virus

Guthrie¹,

Quan²,

Lourens³

et al. 2009

Vaccine

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“…Currently, the use of modified live vector vaccines (MLV) expressing synthetic, codon-optimized antigens which are copies of the naturally encoded genes, are being intensively studied. These have been evaluated in several species for their potential to stimulate both humoral and cell-mediated immune responses against influenza virus [17,[20][21][22]. Viral vectors may be preferred vehicles for heterologous gene delivery as they can induce similar immune responses to those observed during natural infection.…”

Section: Discussionmentioning

confidence: 99%

Evaluation of a vectored equine herpesvirus type 1 (EHV-1) vaccine expressing H3 haemagglutinin in the protection of dogs against canine influenza

Rosas

Walle

Metzger

et al. 2008

Vaccine

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In 2004, canine influenza virus (CIV) was identified as a respiratory pathogen of dogs for the first time and is closely related to H3N8 equine influenza virus (EIV). We generated a recombinant vectored vaccine that expresses H3 of a recent isolate of EIV using equine herpesvirus type 1 (EHV-1) as the delivery vehicle. This EHV-1 vectored vaccine exhibited robust and stable EIV H3 expression and induced a strong influenza virus-specific response in both mice and dogs upon intranasal or subcutaneous administration. Furthermore, upon challenge with the recent CIV isolate A/canine/PA/ 10915-07, protection of vaccinated dogs could be demonstrated by a significant reduction in clinical sings, and, more importantly, by a significant reduction in virus shedding. We concluded that the EHV-1/H3 recombinant vector can be a valuable alternative for protection of dogs against clinical disease induced by CIV and can significantly reduce spread.

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“…В отличие от инактивированных вакцин она способна формировать у привитых лошадей как гу-моральный (включая секреторные IgA антитела), так mir-journal.org Безопасная и эффективная вакцина против гриппа лошадей и клеточный иммунные ответы [13,14]. Однако, как и в случае инактивированных вакцин, для формиро-вания у лошадей протективного иммунного ответа продолжительностью 12 месяцев необходимо трех-кратное введение этой вакцины (первые два -с ин-тервалом в 35 дней и третье -на 6-м месяце) [15]. Более того, ввиду наличия в составе этой вакцины адъюванта Carbormer 974P, она нередко приводит к местным нежелательным явлениям у привитых лошадей [16,17].…”

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“…Еще одним преимуществом двукратной вакцинации по сравнению с однократной является ее способность индуцировать у лошадей выраженную клиническую и вирусологическую защиту от гетерологичного ви-руса дикого типа A/equine/Sydney/2888-8/2007 (Н3N8) через 12 месяцев после повторной иммунизации [30]. Сравнительный анализ полученных результатов и литературных данных [5,15,33,34] показал, что по созданию продолжительного протективного иммун-ного ответа у лошадей живая аттенуированная вакци-на из реассортантного са штамма A/HK/Otar/6:2/2010 превосходит все известные коммерческие вакцины (инактивированные и рекомбинантные векторные) против гриппа лошадей. Полученные результаты дают основание полагать, что разработанная вакцина может составить хорошую альтернативу инактивиро-ванным и рекомбинантным векторным вакцинам, применяемым в Казахстане и других неблагополуч-ных по гриппу лошадей странах.…”

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Новая Безопасная И Эффективная Живая Модифицированная Холодоадаптированная Вирусная Вакцина Против Гриппа Лошадей, Позволяющая Дифференцировать Инфицированных Животных От Вакцинированных

Tabynov¹

2016

Microbiology Independent Research Journal (MIR Journal)

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An analysis of the main advantages and shortcomings of the existing inactivated and live vaccines against the equine influenza viruses is given in this paper. For the first time, the most important information, concerning the development of a new live modified cold-adapted equine influenza virus vaccine based on the A/HK/Otar/6:2/2010 strain is summarized. We discuss a number of unique features of the developed vaccine that have not previously been reported, and compare the new vaccine with the existing equine influenza vaccines. The properties of developed equine vaccine include: long lasting (12 months or more) protective immunity after a single immunization; sterile immunity after double vaccination; cross-protection against the heterologous virus in 12 months after a double vaccination and the differentiation of infected animals from vaccinated animals.Грипп лошадей -остро протекающая контагиозная вирусная болезнь, характеризующаяся катаральным воспалением органов респираторного тракта, общим угнетением, кратковременной лихорадкой и сухим болезненным кашлем, а в тяжелых случаях -разви-тием пневмонии. Среди известных подтипов вируса гриппа лошадей (ВГЛ) Н7N7 и Н3N8 наиболее распро-страненным считается Н3N8, который представляет серьезную угрозу для здоровья лошадей, а также эко-номическую проблему для коневодства [1]. В насто-ящее время наиболее эффективным способом борь-бы против этой инфекции является специфическая

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Efficacy of a canarypox-vectored recombinant vaccine expressing the hemagglutinin gene of equine influenza H3N8 virus in the protection of ponies from viral challenge

Abstract: The rCP-EIV vaccine provided protection of ponies to viral challenge. Of particular importance was the protection at 5 months after the second dose, indicating that this vaccine closes an immunity gap between the second and third vaccination.

Cited by 59 publications

References 25 publications

Protective immunization of horses with a recombinant canarypox virus vectored vaccine co-expressing genes encoding the outer capsid proteins of African horse sickness virus

Protective immunization of horses with a recombinant canarypox virus vectored vaccine co-expressing genes encoding the outer capsid proteins of African horse sickness virus

Evaluation of a vectored equine herpesvirus type 1 (EHV-1) vaccine expressing H3 haemagglutinin in the protection of dogs against canine influenza

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