Publication | Open Access
Role of Sphingomyelinase in Infectious Diseases Caused by Bacillus cereus
66
Citations
40
References
2012
Year
Microbial PathogensBacteriologyImmunologyCell DeathInnate ImmunityBacterial PathogensMedical MicrobiologyPathogen BiologyInfection ControlAntimicrobial ResistanceAerobic CulturingBacillus CereusHealth SciencesMicrobial ToxinVirulence FactorImmune FunctionClinical MicrobiologyPhagocyteMicrobial DiseasePathogenesisB. CereusMouse MacrophagesMicrobiologyMedicineBc-smase Gene
Bacillus cereus (B. cereus) is a pathogen in opportunistic infections. Here we show that Bacillus cereus sphingomyelinase (Bc-SMase) is a virulence factor for septicemia. Clinical isolates produced large amounts of Bc-SMase, grew in vivo, and caused death among mice, but ATCC strains isolated from soil did not. A transformant of the ATCC strain carrying a recombinant plasmid containing the Bc-SMase gene grew in vivo, but that with the gene for E53A, which has little enzymatic activity, did not. Administration of an anti-Bc-SMase antibody and immunization against Bc-SMase prevented death caused by the clinical isolates, showing that Bc-SMase plays an important role in the diseases caused by B. cereus. Treatment of mouse macrophages with Bc-SMase resulted in a reduction in the generation of H(2)O(2) and phagocytosis of macrophages induced by peptidoglycan (PGN), but no effect on the release of TNF-α and little release of LDH under our experimental conditions. Confocal laser microscopy showed that the treatment of mouse macrophages with Bc-SMase resulted in the formation of ceramide-rich domains. A photobleaching analysis suggested that the cells treated with Bc-SMase exhibited a reduction in membrane fluidity. The results suggest that Bc-SMase is essential for the hydrolysis of SM in membranes, leading to a reduction in phagocytosis.
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