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Major histocompatibility complex variation is similar in little brown bats before and after white-nose syndrome outbreak

  • Xueling Yi
  • , Deahn M. Donner
  • , Paula E. Marquardt
  • , Jonathan M. Palmer
  • , Michelle A. Jusino
  • , Jacqueline Frair
  • , Daniel L. Lindner
  • , Emily K. Latch

Research output: Contribution to journalArticlepeer-review

4 Scopus citations

Abstract

White-nose syndrome (WNS), caused by the fungal pathogen Pseudogymnoascus destructans (Pd), has driven alarming declines in North American hibernating bats, such as little brown bat (Myotis lucifugus). During hibernation, infected little brown bats are able to initiate anti-Pd immune responses, indicating pathogen-mediated selection on the major histocompatibility complex (MHC) genes. However, such immune responses may not be protective as they interrupt torpor, elevate energy costs, and potentially lead to higher mortality rates. To assess whether WNS drives selection on MHC genes, we compared the MHC DRB gene in little brown bats pre- (Wisconsin) and post- (Michigan, New York, Vermont, and Pennsylvania) WNS (detection spanning 2014–2015). We genotyped 131 individuals and found 45 nucleotide alleles (27 amino acid alleles) indicating a maximum of 3 loci (1–5 alleles per individual). We observed high allelic admixture and a lack of genetic differentiation both among sampling sites and between pre- and post-WNS populations, indicating no signal of selection on MHC genes. However, post-WNS populations exhibited decreased allelic richness, reflecting effects from bottleneck and drift following rapid population declines. We propose that mechanisms other than adaptive immunity are more likely driving current persistence of little brown bats in affected regions.

Original languageEnglish
Pages (from-to)10031-10043
Number of pages13
JournalEcology and Evolution
Volume10
Issue number18
DOIs
StatePublished - Sep 1 2020

Keywords

  • Myotis lucifugus
  • North American bat
  • Pseudogymnoascus destructans
  • fungal disease
  • immunity
  • major histocompatibility complex

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