Transcriptional Profiles Elucidate Differential Host Responses to Infection with and .

Many aspects of the host response to invasive cryptococcal infections remain poorly understood. In order to explore the pathobiology of infection with common clinical strains, we infected BALB/cJ mice with , , or sham control, and assayed host transcriptomic responses in peripheral blood. Infection with resulted in markedly greater fungal burden in the CNS than , as well as slightly higher fungal burden in the lungs. A total of 389 genes were significantly differentially expressed in response to infection, which mainly clustered into pathways driving immune function, including complement activation and TH2-skewed immune responses. infection demonstrated dramatic up-regulation of complement-driven genes and greater up-regulation of alternatively activated macrophage activity than seen with . A 27-gene classifier was built, capable of distinguishing cryptococcal infection from animals with bacterial infection due to with 94% sensitivity and 89% specificity. Top genes from the murine classifiers were also differentially expressed in human PBMCs following infection, suggesting cross-species relevance of these findings. The host response, as manifested in transcriptional profiles, informs our understanding of the pathophysiology of cryptococcal infection and demonstrates promise for contributing to development of novel diagnostic approaches.