Anthrax toxin targeting of myeloid cells through the CMG2 receptor is essential for establishment of Bacillus anthracis infections in mice

Bacillus anthracis kills through a combination of bacterial infection and toxemia. Anthrax toxin working via the CMG2 receptor mediates lethality late in infection, but its roles early in infection remain unclear. We generated myeloid-lineage specific CMG2-deficient mice to examine the roles of macr...

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Published inCell host & microbe Vol. 8; no. 5; pp. 455 - 462
Main Authors Liu, Shihui, Miller-Randolph, Sharmina, Crown, Devorah, Moayeri, Mahtab, Sastalla, Inka, Okugawa, Shu, Leppla, Stephen H
Format Journal Article
LanguageEnglish
Published United States 18.11.2010
Subjects
Animals
Anthrax - immunology
Anthrax - microbiology
Antigens, Bacterial - metabolism
Bacillus anthracis - metabolism
Bacillus anthracis - pathogenicity
Bacterial Toxins - metabolism
Host-Pathogen Interactions
Macrophages - metabolism
Macrophages - microbiology
Mice
Mice, Inbred C57BL
Myeloid Cells - immunology
Myeloid Cells - metabolism
Myeloid Cells - microbiology
Neutrophils - metabolism
Neutrophils - microbiology
Receptors, Peptide - genetics
Receptors, Peptide - metabolism
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Summary:Bacillus anthracis kills through a combination of bacterial infection and toxemia. Anthrax toxin working via the CMG2 receptor mediates lethality late in infection, but its roles early in infection remain unclear. We generated myeloid-lineage specific CMG2-deficient mice to examine the roles of macrophages, neutrophils, and other myeloid cells in anthrax pathogenesis. Macrophages and neutrophils isolated from these mice were resistant to anthrax toxin. However, the myeloid-specific CMG2-deficient mice remained fully sensitive to both anthrax lethal and edema toxins, demonstrating that targeting of myeloid cells is not responsible for anthrax toxin-induced lethality. Surprisingly, the myeloid-specific CMG2-deficient mice were completely resistant to B. anthracis infection. Neutrophil depletion experiments suggest that B. anthracis relies on anthrax toxin secretion to evade the scavenging functions of neutrophils to successfully establish infection. This work demonstrates that anthrax toxin uptake through CMG2 and the resulting impairment of myeloid cells are essential to anthrax infection.
Bibliography:ObjectType-Article-1
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ISSN:1931-3128
1934-6069
DOI:10.1016/j.chom.2010.10.004