Comparative Studies on Structural and Antigenic Properties of Two Serotypes of Infectious Bursal Disease Virus

Abstract: SUMMARYThe electrophoretic mobilities of the two genome segments and the structural polypeptides of the chicken strain Cu-1 (serotype I) and the turkey isolate 23/82 (serotype II) of infectious bursal disease virus were compared. There is a close antigenic relationship between the smaller of the two major structural proteins (32K) of both strains. Neutralizing monoclonal antibodies are induced by the larger protein (40K in Cu-1) which differentiates between the two serotypes. The 40K structural protein also ha… Show more

“…The numbering of the strains corresponds to that in region covers the C-terminal part of VP2 and the Nterminal part of the NS protein whereas all MAbs developed against IPNV are either VP2-or VP3-specific (Caswell-Reno et al, 1986;Lecomte et al, 1992). Similar data were also obtained with IBDV (Azad et al, 1987;Becht et al, 1988;Fahey et al, 1989;Jagadish & Azad, 1991). Because the precise location of the junction between the two proteins on genome segment A has not yet been determined, it is not possible to calculate the exact proportion of each protein represented in the eDNA fragment.…”

Evidence of genomic variations between infectious pancreatic necrosis virus strains determined by restriction fragment profiles

“…The numbering of the strains corresponds to that in region covers the C-terminal part of VP2 and the Nterminal part of the NS protein whereas all MAbs developed against IPNV are either VP2-or VP3-specific (Caswell-Reno et al, 1986;Lecomte et al, 1992). Similar data were also obtained with IBDV (Azad et al, 1987;Becht et al, 1988;Fahey et al, 1989;Jagadish & Azad, 1991). Because the precise location of the junction between the two proteins on genome segment A has not yet been determined, it is not possible to calculate the exact proportion of each protein represented in the eDNA fragment.…”

Evidence of genomic variations between infectious pancreatic necrosis virus strains determined by restriction fragment profiles

“…Protection against IBDV is considered to be chiefly antibody mediated. The major host protective immunogen of IBDV (VP2) contains at least two or three closely-linked antigenic sites capable of inducing virus-neutralizing antibodies in chickens (Becht et al, 1988). Vaccination with VP2 expressed in prokaryotic and eukaryotic vectors is capable of eliciting neutralizing antibodies in chickens, and chickens are protected against clinical disease and mortality following challenge but not against bursal damage (Dybing & Jackwood, 1998).…”

T-Cell suppression by cyclosporin-A enhances infectious bursal disease virus infection in experimentally infected chickens

“…VP3 has been used to induce antibodies but these were only very weakly neutralizing (Fahey et aL, 1985b). Monoclonal antibodies (MAbs) have been raised against VP2 and VP3, but only those reacting to VP2 have the ability to neutralize the virus (Azad et al, 1987;Becht et al, 1988;Snyder et al, 1988). One neutralizing MAb recognition site has been mapped to a specific region of VP2 between amino acids 206 and 350 (Azad et al, 1987).…”

“…Neutralizing antibodies are elicited by VP2 (Becht et al, 1988;Fahey et al, 1989). VP3 has been used to induce antibodies but these were only very weakly neutralizing (Fahey et aL, 1985b).…”

A comparison of the sequences of segment A of four infectious bursal disease virus strains and identification of a variable region in VP2