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A Murine Model for Disseminated Candidiasis in Neonates

机译:小鼠模型播散性念珠菌病新生儿

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摘要

Candida albicans is the leading fungal pathogen causing invasive disease in immunocompromised patients including the neonate. A reliable animal model for disseminated candidiasis in the neonate is needed to study the unique aspects of this host-pathogen interaction. To establish such a model, two day old BALB/c mouse pups were given intraperitoneal injections with varied inocula of C. albicans or saline control. Pups were examined every 3-8 hours for death. Surviving pups were sacrificed at 72 hours. Kidney, lung, spleen, liver and brain were homogenized and plated for colony counts and/or fixed for histological staining. Intraperitoneal injection of C. albicans led to mortality in a dose-dependent fashion. Disseminated infection was confirmed by colony counts of homogenized kidney, lung, and brain, as well as by histological examination. Infection with a C. albicans mutant lacking the cell surface adhesin, Als3p, led to significant reduction in mortality relative to wild-type (P = 0.03). This model will be useful to study the unique aspects of antifungal defense in a neonatal host and will provide a means to test novel therapeutic strategies.

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