The N545S and K717N substitution at the N-glycosylation sites of the S2 subunit of avian infectious bronchitis virus can significantly enhance viral pathogenicity.

Publication date: Sep 01, 2024

The S2 subunit of infectious bronchitis virus (IBV) is a heavily glycosylated protein that can impact various characteristics of the virus. It is currently known that N-glycosylation modifications are predominantly located on the S2 subunit. However, the exact role of their N-glycosylation modification remains undisclosed. To elucidate the function of these N-glycosylation sites, we identified 14 common sites distributed on the S2 subunit of the 5 genotypes of IBV in present study. Subsequently, we selected 7 sites to generate mutants and assessed their impact on viral virulence, replication ability, and antigenicity. Our finding revealed that only 2 substitutions, N545S and K717N, increased the viral replication titer and antigenicity, and ultimately the pathogenicity in chicks. To delve into the mechanisms underlying this increased pathogenicity, we discovered that K717N can change the structure of antigenic epitopes. The N545S substitution not only influenced antigenic epitope structure, but also enhanced the ability of the virus to enter CEKs during the early stages of viral replication. These results suggest that the enhanced viral pathogenicity associated with N545S and K717N substitutions is multifaceted, with acceleration of the viral membrane fusion process and alterations in epitope structure representing crucial factors in the capability of N-glycosylation modifications to boost viral virulence. These insights provide valuable guidance for the efficient development of live attenuated vaccines.

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Concepts Keywords
Avian Amino Acid Substitution
Efficient Animals
Mutants Chickens
N545s Coronavirus Infections
Vaccines Glycosylation
Infectious bronchitis virus
infectious bronchitis virus
N-glycosylation
pathogenicity
Poultry Diseases
S2 subunit
Virulence
Virus Replication

Semantics

Type Source Name
disease VO Infectious bronchitis virus
disease IDO virulence
disease IDO replication
pathway KEGG Viral replication
disease VO titer
disease IDO process
disease VO efficient
disease MESH Coronavirus Infections
disease MESH Poultry Diseases

Original Article

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