Protective role of Bacillus anthracis exosporium in macrophage-mediated killing by nitric oxide.

نویسندگان

  • John Weaver
  • Tae Jin Kang
  • Kimberly W Raines
  • Guan-Liang Cao
  • Stephen Hibbs
  • Pei Tsai
  • Les Baillie
  • Gerald M Rosen
  • Alan S Cross
چکیده

The ability of the endospore-forming, gram-positive bacterium Bacillus anthracis to survive in activated macrophages is key to its germination and survival. In a previous publication, we discovered that exposure of primary murine macrophages to B. anthracis endospores upregulated NOS 2 concomitant with an .NO-dependent bactericidal response. Since NOS 2 also generates O(2).(-), experiments were designed to determine whether NOS 2 formed peroxynitrite (ONOO(-)) from the reaction of .NO with O(2).(-) and if so, was ONOO(-) microbicidal toward B. anthracis. Our findings suggest that ONOO(-) was formed upon macrophage infection by B. anthracis endospores; however, ONOO(-) does not appear to exhibit microbicidal activity toward this bacterium. In contrast, the exosporium of B. anthracis, which exhibits arginase activity, protected B. anthracis from macrophage-mediated killing by decreasing .NO levels in the macrophage. Thus, the ability of B. anthracis to subvert .NO production has important implications in the control of B. anthracis-induced infection.

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عنوان ژورنال:
  • Infection and immunity

دوره 75 8  شماره 

صفحات  -

تاریخ انتشار 2007