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Peer-reviewed veterinary case report

Transcriptional profiles of vaccine-induced protection in bovine herpesvirus-1 and-challenged bison.

Journal:
Frontiers in veterinary science
Year:
2025
Authors:
Goldkamp, Anna K et al.
Affiliation:
United States Department of Agriculture · United States

Abstract

INTRODUCTION: causes chronic respiratory disease with high mortality rates in American bison (). A recent study showed that a subunit vaccine containingelongation factor thermal unstable (EFTu) and heat shock protein 70 (Hsp70) antigens induced immunity and enhanced protection in bison, resulting in reduced lung lesions and bacterial loads following experimentalchallenge. This study aimed to characterize the transcriptional responses underlying this protection in vaccinated ( = 5) compared to unvaccinated control ( = 4) bison followinginfection. METHODS: Two doses of vaccines were administered on day 0 and at 21 days post-vaccination (DPV), followed by intranasal inoculation with bovine herpesvirus-1 (BHV-1) at 36 DPV andat 40 DPV. RNA sequencing was performed on liver, palatine tonsil (PT), retropharyngeal lymph node (RPLN), tracheobronchial lymph node (TBLN), spleen, and whole blood samples. Blood was collected at 1st vaccination (Day 0), 2nd vaccination (21 days post-vaccination), BHV-1 inoculation (36 DPV),inoculation (40 DPV), and 1 week postinoculation (47 DPV). RESULTS AND DISCUSSION: The greatest number of differentially expressed transcripts (DETs) (≤0.05 FDR) were found in blood at 36 DPV (123 total DETs) and in spleen (57 DETs). At 36 DPV, vaccinated animals showed upregulation of transcripts involved in in cell adhesion, T-helper cell (Th1/Th2/Th17) differentiation, and antigen processing and presentation. This signifies a robust response to the 2nd vaccine dose, which caused increased expression of,, andcorrelating to increased T cell proliferation. Notably, transcription factorsandwere upregulated in vaccinated animals. Spleen-specific regulation included transcripts involved in innate immune response, such asand. These findings highlight the robust immune response induced by the vaccine, particularly through T-cell mediated responses, demonstrating its potential to enhance protective immunity againstin bison.

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Original publication: https://pubmed.ncbi.nlm.nih.gov/41036542/