A variety of animal models have been used to investigate the virulence and pathogenicity of Lichtheimia species. Like in mice, intravenous infection leads to the development of disease and mortality in healthy rabbits and bank voles with kidney and brain being the main target organs.[77, 78] Intranasal infection of bank voles did only rarely lead to mortality but fungi disseminated and could be isolated from lung, liver, brain and kidney at high infection doses.[78] In contrast, intratracheal infection of Asian water buffalo calves led to restricted, self-limiting lung infection without fatalities and dissemination.[79] These results demonstrate that Lichtheimia can infect a wide
range of host species but that disease
development depends on the route of infection and immunosuppression. KU-57788 cost Due to ethical and practical limitations of the use of mammals as infection models to analyse virulence in large numbers of strains, an alternative infection model using chicken embryos has been developed for different bacteria and fungi, including Lichtheimia.[25, 80-82] To study virulence of Lichtheimia species, infection was performed via the chorioallantoic membrane.[25] The main features of infection in this model were penetration and destruction of blood vessels, comparable to human disease. Mortality and the extend of pathological alterations were higher in the clinical-relevant Erlotinib mouse species L. corymbifera, L. ramosa and L. ornata compared to the non-clinical species L. hyalospora and L. sphaerocystis, suggesting that the different Lichtheimia species exhibit differences in their virulence potential.[25] In summary, Abiraterone in vitro Lichtheimia species (especially L. ramosa and L. corymbifera) are important causes of mucormycoses. The clinical disease resembles infections with other mucoralean fungi; however, it remains unclear whether the same predisposing risk factors underlie mucormycoses caused by the different
genera and species. Further epidemiological studies are needed to address these questions. Furthermore, the elucidation of pathogenesis mechanisms, assessment of risk factors and determination of the relative virulence of the different Lichtheimia species and strains would greatly benefit from the development of standardised mammalian infection models. The authors declare that no conflict of interest exists. “
“Considerable changes in the dermatophyte spectrum have been observed in the past century. Hence, many authors point out the necessity of performing periodical overviews of the mycological flora producing mycoses in humans in a given area. Analysis of dermatophyte species was performed, which were isolated from the lesions in patients suspected of superficial mycosis and referred to the Department of Mycology. The materials were isolated from patients suspected of superficial mycosis from Kraków region from January 1, 1972 through December 31, 2007.