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Title: Temperature‐mediated shifts in salamander transcriptomic responses to the amphibian‐killing fungus
Abstract

Life processes of ectothermic vertebrates are intimately linked to the temperature of their environment, influencing their metabolism, reproduction, behaviour and immune responses. In amphibians infected by the generalist chytrid pathogenBatrachochytrium dendrobatidis(Bd), host survival, infection prevalence and infection intensity are often temperature‐ and/or seasonally dependent. However, the transcriptional underpinnings of thermal differences in infection responses remain unknown. Measuring the impact of temperature on host responses to infection is a key component for understanding climatic influences on chytrid disease dynamics. TheBd‐responsive gene pathways in frogs are well documented, but our understanding of salamander immune expression profiles during infection with chytrids remains limited. Here we characterize the transcriptomic responses ofPlethodon cinereususing RNA sequencing by comparing skin and splenic gene expression of individuals uninfected, succumbing toBdinfection and naturally cleared ofBdinfection at three temperatures. We suggest that amphibian temperature‐dependent susceptibility toBdis probably driven by shifts in expression of the innate and adaptive immune axes. Our study shows increased expression of transcripts associated with inflammation at lower temperatures and a shift towards increased expression of adaptive immune genes, including MHC (major histocompatibility complex), at higher temperatures. In the face of climate change, and as concerns for the spread of emergent chytrid pathogens increase, our results provide important functional genomic resources to help understand how these pathogenic fungi may continue to affect amphibian communities globally in the future.

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NSF-PAR ID:
10458854
Author(s) / Creator(s):
 ;  ;  ;  
Publisher / Repository:
Wiley-Blackwell
Date Published:
Journal Name:
Molecular Ecology
Volume:
29
Issue:
2
ISSN:
0962-1083
Page Range / eLocation ID:
p. 325-343
Format(s):
Medium: X
Sponsoring Org:
National Science Foundation
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