Bighorn sheep T2T genome assembly reveals differences in immune genes: a potential cause of high morbidity due to respiratory pathogens

  1. Temitayo A Olagunju
  2. Mariia Pospelova
  3. John C. Schwartz
  4. Michelle R. Mousel
  5. Lindsay M.W. Piel
  6. Paige C. Grossman
  7. Kathryn P. Huyvaert
  8. Kristen L. Kuhn
  9. Tajbir Raihan
  10. Morgan R. Stegemiller
  11. Sarem F. Khilji
  12. Gordon K. Murdoch
  13. Ahmed Tibary
  14. Lisette P. Waits
  15. Arang Rhie
  16. Sergey Koren
  17. Adam M. Phillippy
  18. Stephanie D. McKay
  19. Shannon M. Clarke
  20. Emily L. Clark
  21. Rudiger Brauning
  22. Noelle E. Cockett
  23. John A. Hammond
  24. Maggie Highland
  25. Yana Safonova
  26. Timothy P.L. Smith
  27. Benjamin D. Rosen
  28. Brenda M. Murdoch
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Abstract

The bighorn sheep (Ovis canadensis), despite its close relation to domestic sheep, suffer higher morbidity and mortality from respiratory disease complexes, likely due to genetic differences in immune responses. Unraveling highly repetitive regions such as immune loci and genetic differences was problematic until now. We generated a bighorn sheep telomere-to-telomere assembly, adding 14.28% of novel sequence compared to the previous reference. This enabled the first complete immune loci annotation revealing the IGL and TR loci are significantly short in bighorn sheep. Importantly, a critical immune gene GBP5 and ZNF501, involved in Golgi-mediated immune response, are lacking in bighorn but present in domestic sheep. Re-analysis of a Mycoplasma ovipneumoniae carriage study, using this assembly, identified the immune gene CAPN2 as a key genetic marker for disease carriage, not observable in the original study. This work provides a critical resource for identifying phenotype-linked genetic variation and exploring evolutionary adaptations of bighorn sheep.

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