001) as did the prevalence of grade III–IV GVHD after HSCT (16–37

001) as did the prevalence of grade III–IV GVHD after HSCT (16–37%, P = 0.006).

Antemortem IFI diagnosis improved during the study from 16% in 1989–1993 to 51% in 2004–2008, (P < 0.001). The rate of breakthrough infections declined from 1994 to 2008 (71–56%, P < 0.001). Most IFIs during later periods of the study were associated with concomitant bacterial infection (64%). Notably, death attributed to the IFI remained at as stable rate during the first 15 years of the autopsy records (70–80%), but decreased to 49% in 2004–2008, (P < 0.001). The prevalence of various fungal pathogens identified at autopsy in patients with haematological malignancies selleck chemicals llc changed significantly over the 20 years of autopsy records (Fig. 1). Aspergillus or presumed Aspergillus spp. (culture negative hyalohyphomycetes) accounted for the majority of infections during all the periods of the study, but declined after 2004 from 0.14 cases per 100 autopsies to 0.06, (P = 0.01). Similarly, the prevalence

of Candida infections decreased from 0.10 cases per 100 autopsies to 0.02, but rebounded in 2004–2008 to 0.05/100 autopsies (P = 0.01). Concurrent Aspergillus and Candida infections also decreased during the study period (P = 0.02). Fusarium infections were 10–50-fold less common than Aspergillus infections and decreased from 0.008 cases per 100 autopsies to 0.003 per 100 autopsies in 2004–2008, (P = 0.08). Mucormycosis was the only mould infection whose prevalence increased over the study period, from 0.006 cases per 100 autopsies in 1989–1993 to 0.018 cases in 2004–2008 (P = 0.04). Other fungal infections including Pneumocystis jiroveci (eight cases alone, two mixed with Candida), histoplasmosis PF-02341066 concentration (three cases), Cryptococcus neoformans (two cases) and phaeohyphomycosis (five cases alone, two mixed with other fungal pathogens) were detected sporadically at low rates in autopsy patients over the 20-year study period. Most mould infections

Isoconazole reported at autopsy as aspergillosis were based on histopathology only, without definitive culture-based identification (Table 2). Among microbiologically documented infections at autopsy, the percentage of infections attributable to A. fumigatus increased over the study period, whereas infections due to other species such as A. flavus, A. terreus and A. niger decreased, although the small numbers limit analysis of the trends. Microbiologically documented Fusarium spp. infections remained relatively constant over the 20-year survey. However, cultures of Mucorales increased fourfold over the 20 year study period, (P = 0.04). Most yeast infections (55%) during the first 5 years of the autopsy survey were based on histopathological evidence of invasion without accompanying culture information. However, histopathological identification lacking culture decreased during the study period representing only 5% of cases by 2004/2008, (P < 0.001). Among monomicrobial culture-documented infections (Table 3), C.

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