A STUDY ON HOMOLOGY AND HETEROLOGY BETWEEN PANASIA-II & PAK-98 LINEAGES OF FOOT AND MOUTH DISEASE VIRUS SEROTYPE-O
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Abstract
To understand the dynamics of epidemics, it is crucial to evaluate prior exposure to infectious diseases as a possible defense against newly developing strains. The cross-protection prediction is unresolved matter that holds great importance, particularly in the field of Foot-and-Mouth Disease Virus (FMDV). The new methods for controlling FMD involve the implementation of vaccine, limited movement, containment and elimination of cattle that are either affected or vulnerable to the disease. Therefore, it is necessary to use a serological analysis strategy that applies association coefficients (r1-values) to identify effective vaccines. The primary objective of this study was aimed to explain the genetic homologous and heterologous association among two ancestries of FMDV serotype O found in Pakistan (Pk) and to find a suitable strain from field for selection of vaccinated seed that provide cross-protection against both ancestries. Virus neutralization tests (VNTs) were used to evaluate an antigenic association among the two groups of viruses, indicates a significant degree of antigenic similarity between stains within a particular cluster. Conversely, r1 values ranging from 0.07-0.2 were obtained from cross-combinations among clusters, suggesting antigenic variation amongst virus strains. These results were further supported by in vitro tests, which showed that heterologous combinations of PanAsia-II and PAK-98 isolates showed antigenic variation, except for 25-06-PK-19, SDG-43-FSD-PK, and TANWL-34PK, which showed a 0.3 (r1 value). In contrast, when considering homologous combination of strains from both lineages showed antigenic similarity. Furthermore, it was projected that these combinations would provide protective titers during in-vivo. As a conclusion, it is recommended that all strains, except 25-06-PK-19, SDG-43-FSD-PK, and TANWL-34PK considered as potential vaccine candidates for effectively managing outbreaks of FMDV serotype-O, due to their ability to confer broad-spectrum immunity.