PLoS ONE (Jan 2012)

Role of sphingomyelinase in infectious diseases caused by Bacillus cereus.

  • Masataka Oda,
  • Manabu Hashimoto,
  • Masaya Takahashi,
  • Yuka Ohmae,
  • Soshi Seike,
  • Ryoko Kato,
  • Aoi Fujita,
  • Hideaki Tsuge,
  • Masahiro Nagahama,
  • Sadayuki Ochi,
  • Teppei Sasahara,
  • Shunji Hayashi,
  • Yoshikazu Hirai,
  • Jun Sakurai

DOI
https://doi.org/10.1371/journal.pone.0038054
Journal volume & issue
Vol. 7, no. 6
p. e38054

Abstract

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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.