5524
Asmaa Mahmoud Mohammed Mohammed Maatouq
Studies On Combined Infection With Low Pathogenic Avian Influenza (H9N2) And Newcastle Disease Genotype VII In Chickens
H9N2, NDV genotype VII, co-infection, RT-PCR, phylogenecity vaccines, HI titres,
Co -infections of Newcastle disease (ND) and avian influenza (AI) were the major viruses causing high mortality and high economic losses. In this study 300 samples were collected from 50 chickens flocks suffering from respiratory symptoms , sever drop in egg production and mortalities from December,2013 to December, 2014. RT-PCR was performed to detect the M protein of H9 gene of avian influenza and F gene of velogenic NDV (vNDV) coinfections. H9 PCR results were 20 and 34 in coloacal and pharyngeal swabs with total percentage of 6.7 % and 11.3%; respectively. The H9 sequences showed low pathogenic RSSR/GLF motif. The phylogenetic tree showed that H9 sequences belong to the G1 lineage which clustered with 2015 -2016 Egyptian H9N2. Partial sequences of the Fusion gene revealed that the isolated NDV isolates belong to class II genotype VIIj. The cleavage site of the F protein showed the presence of a polybasic amino acid motif (112RRQKRF117) suggesting that our two isolates were vNDV strain. Out of molecular identified H9 (1 isolate) and NDV Genotype VII (2 isolates) selected from were named AI/CHICKEN/EGYPT/48Ob/NRC-CU/2014(H9) , NDV/CHICKEN/EGYPT/48Ob/NRCCU/2014 , and NDV/CHICKEN/EGYPT/66Oc/NRC-CU/2014 , and nucleotide sequences were submitted to GenBank and given accession numbers MG966504, MG966505, and MG966506; respectively. In This study we detect levels of protection induced by the commercial ND genotype II Hitchner B1, LaSota vaccination regime and inactivated H9N2 against challenge with vNDV, H9N2 separate and co-infection under experimental condition. Newcastle disease (ND) HI (log2) mean titers in group received NDV vaccines 4.5 ± 1.2, 3.6 ± 1.1 and 4.0 ± 0.4) at 14, 21 and 29 days of age, respectively. Chicken group received ND vaccine and inactivated H9 showed relatively higher HI titres (5.0 ± 1.5, 3.5 ± 1.4 and 4.5 ± 1.3). HI titres against H9N2 in group given H9N2 inactivated vaccine are 3.7 ± 1.6, 2.5 ± 1.1 and 5.1 ± 1.3 at 14, 21 and 29 days; respectively. Challenge with NDV genotype VII at 33 days of age resulted in 100% mortality with severe signs as well as in non-vaccinated control sub-group challenged and 100% mortalities. Sub-groups (2a and 3a) vaccinated with ND vaccine and ND vaccine + H9N2 showed signs of depression, off food and moderate respiratory signs with protection rates is 70 and 75%; respectively. Control group challenged with H9N2 showed general signs with mild respiratory signs and 10% mortalities while, sub-groups given ND vaccine + H9N2 and challenged with H9N2 show 100% survival. Chicken sub-groups vaccinated with ND vaccine or ND vaccine 2+ H9N2 and challenged with NDV+ H9N2 (Co-infection) show signs form the 3rd dpi with moderate respiratory signs and protection rate of 70%; respectively. Post-mortem lesions in vNDV challenged birds were septicemia, intestinal and respiratory lesion, while those challenged with both NDV and H9N2 showed more prominent lesions. The vaccinated groups showed unsatisfactory protection rates (75%). Simultaneous chicken challenge with H9N2 and vNDV pointed out that co-infection increased severity of clinical signs, mortality and gross lesions. No difference in virus shedding of vNDV were found among control unvaccinated and vaccinated groups. All groups shed virus in cloacal and oral swabs at days 4, 6 and 8 post challenge Histopathological changes were reported in lung, intestine, and spleen of challenged non-vaccinated and vaccinated groups. The severity of tissue alteration was remarkably high in the non-vaccinated group and slightly mild tissue alteration in the vaccinated group. The histological changes ranged from severe congestion in blood vessels in tested organ with lymphoid depletion in spleen and hyperplasia of mucosal-associated lymphoid tissue in the intestine. With partial limited tissue change in the challenged vaccinated group.
2018
Ph.d
Cairo
Veterinary Medicine