Abstract

Severe hepatitis-hydropericardium syndrome (HHS) associated with a novel viral genotype, fowl adenovirus 4 (FAdV-4), has emerged and widely spread in China since 2015, causing severe economic losses to the poultry industry. We previously reported that the hexon gene is responsible for pathogenicity and obtained a non-pathogenic hexon-replacement rHN20 strain; however, the lack of information about the non-essential regions for virus replication limits the development of a FAdV-4 vector. This study first established an enhanced green fluorescent protein (EGFP)-indicator virus based on the FAdV-4 reverse genetic technique, effective for batch operations in the virus genome. Based on this, 10 open reading frames (ORFs) at the left end and 13 ORFs at the right end of the novel FAdV-4 genome were deleted separately and identified as non-essential genes for viral replication, providing preliminary insertion sites for foreign genes. To further improve its feasibility as a vaccine vector, seven combinations of ORFs were successfully replaced with EGFP without affecting the immunogenicity of the vector backbone. Finally, a recombinant rHN20-vvIBDV-VP2 strain, expressing the VP2 protein of very virulent infectious bursa disease virus (vvIBDV), was rescued and showed complete protection against FAdV-4 and vvIBDV. Thus, the novel FAdV-4 vector could provide sufficient protection for HHS and efficient exogenous gene delivery. Overall, our findings systemically identified 23 non-essential ORFs for FAdV-4 replication and seven foreign gene insertion regions, providing valuable information for an in-depth understanding of the novel FAdV-4 pathogenesis and development of multivalent vaccines.

Highlights

  • Adenoviruses are non-enveloped, double-stranded DNA viruses that infect multiple vertebrates, including mammals, birds, fish, and reptiles (Greber, 2020)

  • Seven combinations of open reading frames (ORFs) were successfully replaced with enhanced green fluorescent protein (EGFP) without affecting the immunogenicity of the vector backbone

  • We systematically identified all ORFs located at both ends of the emerging novel fowl adenovirus 4 (FAdV-4) genome as nonessential genes for virus replication

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Summary

Introduction

Adenoviruses (family Adenoviridae) are non-enveloped, double-stranded DNA viruses that infect multiple vertebrates, including mammals, birds, fish, and reptiles (Greber, 2020). A severe outbreak of HHS by the novel FAdV-4 has occurred in China since 2015, causing severe economic losses to the poultry industry (Liu et al, 2016; Niu et al, 2016; Xia et al, 2017; Li et al, 2018). Human adenovirus vectors have been widely used for gene therapy (Arnone et al, 2021) and vaccines against emergent viruses such as Ebola (Li et al, 2017) and SARS-Cov-2 (Tostanoski et al, 2021), non-human and non-mammalian adenoviruses, including FAdVs, are used less frequently as vectors

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