Transcriptomic Analysis of Circulating Leukocytes Obtained during the Recovery from Clinical Mastitis Caused by Escherichia coli in Holstein Dairy Cows

Zhangrui Cheng; Sergio Palma-Vera; Laura Buggiotti; Mazdak Salavati; Frank Becker; Dirk Werling; D Claire Wathes; GplusE Consortium

doi:10.3390/ani12162146

Transcriptomic Analysis of Circulating Leukocytes Obtained during the Recovery from Clinical Mastitis Caused by Escherichia coli in Holstein Dairy Cows

Animals (Basel). 2022 Aug 21;12(16):2146. doi: 10.3390/ani12162146.

Authors

Zhangrui Cheng¹, Sergio Palma-Vera², Laura Buggiotti¹, Mazdak Salavati¹, Frank Becker², Dirk Werling^{1

3}, D Claire Wathes¹, GplusE Consortium

Affiliations

¹ Department for Pathobiology and Population Sciences, Royal Veterinary College, Hatfield AL9 7TA, UK.
² Research Institute for Farm Animal Biology, Wilhelm-Stahl-Allee 2, 18196 Dummerstorf, Germany.
³ Centre for Vaccinology and Regenerative Medicine, Royal Veterinary College, Hatfield AL9 7TA, UK.

Abstract

The risk and severity of clinical infection with Escherichia coli as a causative pathogen for bovine mastitis is influenced by the hosts' phenotypic and genotypic variables. We used RNA-Seq analysis of circulating leukocytes to investigate global transcriptomic profiles and genetic variants from Holstein cows with naturally occurring cases of clinical mastitis, diagnosed using clinical symptoms and milk microbiology. Healthy lactation-matched cows served as controls (CONT, n = 6). Blood samples were collected at two time periods during the recovery phase post diagnosis: EARLY (10.3 ± 1.8 days, n = 6) and LATE (46.7 ± 11 days, n = 3). Differentially expressed genes (DEGs) between the groups were identified using CLC Genomics Workbench V21 and subjected to enrichment analysis. Variant calling was performed following GATKv3.8 best practice. The comparison of E. coli(+) EARLY and CONT cows found the up-regulation of 1090 DEGs, mainly with immune and inflammatory functions. The key signalling pathways involved NOD-like and interleukin-1 receptors and chemokines. Many up-regulated DEGs encoded antimicrobial peptides including cathelicidins, beta-defensins, S100 calcium binding proteins, haptoglobin and lactoferrin. Inflammation had largely resolved in the E. coli(+) LATE group, with only 29 up-regulated DEGs. Both EARLY and LATE cows had up-regulated DEGs encoding ATP binding cassette (ABC) transporters and haemoglobin subunits were also up-regulated in LATE cows. Twelve candidate genetic variants were identified in DEGs between the infected and CONT cows. Three were in contiguous genes WIPI1, ARSG and SLC16A6 on BTA19. Two others (RAC2 and ARHGAP26) encode a Rho-family GTPase and Rho GTPase-activating protein 26. These results show that the initial inflammatory response to E. coli continued for at least 10 days despite prompt treatment and provide preliminary evidence for genetic differences between cows that may predispose them to infection.

Keywords: ABC transporters; E. coli mastitis; MHC system; antimicrobial peptides; cow; mammary gland.

Grants and funding

613689/European Union's Seventh Framework Programme (Brussels, Belgium) for research, technological development, and demonstration