Whole Transcriptome Analysis of Host and Pathogen Gene Expression in White-Nose Syndrome


Meeting Abstract

16-5  Monday, Jan. 4 11:15  Whole Transcriptome Analysis of Host and Pathogen Gene Expression in White-Nose Syndrome FIELD, KA*; JOHNSON, JS; LILLEY, TM; REEDER, SM; ROGERS, EJ; BEHR, MJ; REEDER, DM; Bucknell University; Bucknell University; Bucknell University; Bucknell University; Bucknell University; University of Wisconson; Bucknell University kfield@bucknell.edu http://fieldresearchlab.blogs.bucknell.edu

White-nose syndrome (WNS) in North American bats is caused by an invasive cutaneous infection by the psychrophilic fungus Pseudogymnoascus destructans (Pd). We compared transcriptome-wide changes in gene expression using RNA-Seq on wing skin tissue from hibernating little brown myotis (Myotis lucifugus) with WNS to bats without Pd exposure. We found that WNS caused significant changes in gene expression in hibernating bats including pathways involved in inflammation, wound healing, and metabolism. Local acute inflammatory responses were initiated by fungal invasion. Gene expression was increased for inflammatory cytokines, including interleukins (IL) IL-1β, IL-6, IL-17C, IL-20, IL-23A, IL-24, and G-CSF and chemokines, such as Ccl2 and Ccl20. This pattern of gene expression changes demonstrates that WNS is accompanied by an innate anti-fungal host response similar to that caused by cutaneous Candida albicans infections. However, despite the apparent production of appropriate chemokines, immune cells such as neutrophils and T cells do not appear to be recruited. We observed upregulation of acute inflammatory genes, including prostaglandin G/H synthase 2 (cyclooxygenase-2), that generate eicosanoids and other nociception mediators. We also identified several classes of potential virulence factors that are expressed in Pd during WNS, including secreted proteases that may mediate tissue invasion. These results demonstrate that hibernation does not prevent a local inflammatory response to Pd infection but that recruitment of leukocytes to the site of infection does not occur. These observations support a dual role for inflammation during WNS; inflammatory responses provide protection but excessive inflammation may contribute to mortality.

the Society for
Integrative &
Comparative
Biology