Susceptibility of vaccinated and unvaccinated Egyptian chickens to very virulent infectious bursal disease virus

Hassan, Mohamed K.; Afify, Mohamed; Aly, Mona M.

doi:10.1080/03079450120118630

Cited by 31 publications

(11 citation statements)

References 23 publications

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“…These strains can cause lesions typical of IBDV and are antigenically similar to the classical strains (Eterradossi et al, 1992). Remarkably, however, vvIBDV can establish infection in the face of maternally derived antibodies as well as antibody levels after vaccination that were previously protective against classical strains (Hassan et al, 2002). Meanwhile vvIBDV infections also have been observed in Africa, Asia (for example, Eterradossi et al, 1999;Zierenberg et al, , 2001Parede et al, 2003;van den Berg et al, 2004) and in South America (Ikuta et al, 2001), but not in Australia (Sapats & Ignjatovic, 2002).…”

Section: Reversion Of Molecularly Engineered Partially Attenuated Vmentioning

confidence: 94%

Reversion of molecularly engineered, partially attenuated, very virulent infectious bursal disease virus during infection of commercial chickens

Raue

Islam

et al. 2004

Avian Pathology

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A molecularly cloned, tissue culture-adapted infectious bursal disease virus (BD-3tc) was generated from a very virulent strain by the reverse genetics approach following site-directed mutagenesis (Q253H and A284T in VP2). The pathogenicity of BD-3tc was tested in commercial chickens. The wild-type strain (BD-3wt) and the molecularly cloned parental strain (BD-3mc) were included for comparison. The subclinical course of the disease, with delayed and milder pathological lesions followed by quick follicular regeneration in the bursa of Fabricius in BD-3tc-inoculated birds, suggested that these amino acid substitutions made BD-3tc partially attenuated. However, severe bursa atrophy was observed at 14 days after inoculation. Reverse transcription-polymerase chain reaction coupled with restriction enzyme analysis revealed that both point mutations in BD-3tc had reverted 14 days after inoculation. Further investigations demonstrated that the codon for amino acid at position 284 had already reverted to the wild-type phenotype (T284A) 3 days after inoculation.

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Section: Reversion Of Molecularly Engineered Partially Attenuated Vmentioning

confidence: 94%

Reversion of molecularly engineered, partially attenuated, very virulent infectious bursal disease virus during infection of commercial chickens

Raue

Islam

et al. 2004

Avian Pathology

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“…The 99323 isolate was identified from Egypt during a worldwide survey of antigenic variation among IBDV strains causing acute IBD outbreaks. Such outbreaks have been reported to be a cause for continuing problems in the field in Egypt since the early 1990s, in spite of extensive and multiple administrations of live vaccines with various degrees of attenuation (Hassan et al, 2002). The 28% mortality induced by isolate 99323 following an experimental 10 4.24 EID 50 challenge in SPF chickens (not significantly different from that induced by strain 89163), the presence in the VP2 protein of 99323 of the four aa found in the typical vvIBDV, and the genetic relatedness between the nt sequences of 99323 and of typical vvIBDVs (as demonstrated by high bootstrap values in the consensus trees) all corroborate the fact that isolate 99323 is indeed a vvIBDV.…”

Section: Discussionmentioning

confidence: 99%

Extensive antigenic changes in an atypical isolate of very virulent infectious bursal disease virus and experimental clinical control of this virus with an antigenically classical live vaccine

Eterradossi¹,

Gauthier²,

Reda³

et al. 2004

Avian Pathology

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“…Similarly spleen:body weight ratios are also used to assess spleenic atrophy (Hassan et al, 2002). The term bursal index is used to indicate the ratio obtained by dividing the BB ratio of infected/ vaccinated chickens by the BB ratio of uninfected/ unvaccinated chickens.…”

Section: Introductionmentioning

confidence: 99%

Egg:embryo weight ratio as an indicator of dwarfism induced by infectious bronchitis virus

et al. 2004

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A simple objective method to quantify embryo dwarfism induced by infectious bronchitis virus in embryonated chicken eggs has been used to determine endpoints in virus titration and neutralization assays. The eggs and the respective embryos were weighed and embryo:egg weight (EE) ratios were calculated. The EE ratios were compared with the uninoculated control eggs and endpoints could be calculated objectively. EE indices were also calculated by dividing the EE ratios of inoculated embryonated chicken eggs by the mean EE ratio of uninoculated controls, or in the case of virus neutralization tests by the mean EE ratio of eggs inoculated with virus alone. Although this mean EE index did not reflect the dwarfing (or lack of it) in individual eggs, it served as a group indicator. This method would be useful to observe embryo lesions especially in field (non-egg adapted) infectious bronchitis virus isolates, which does not cause observable dwarfing until several embryo passages.

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Susceptibility of vaccinated and unvaccinated Egyptian chickens to very virulent infectious bursal disease virus

Cited by 31 publications

References 23 publications

Reversion of molecularly engineered, partially attenuated, very virulent infectious bursal disease virus during infection of commercial chickens

Reversion of molecularly engineered, partially attenuated, very virulent infectious bursal disease virus during infection of commercial chickens

Extensive antigenic changes in an atypical isolate of very virulent infectious bursal disease virus and experimental clinical control of this virus with an antigenically classical live vaccine

Egg:embryo weight ratio as an indicator of dwarfism induced by infectious bronchitis virus

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