Metal Chelation and Inhibition of Bacterial Growth in Tissue Abscesses

Brian D. Corbin; Erin H. Seeley; Andrea Raab; Jörg Feldmann; Michael R. Miller; Victor J. Torres; Kelsi L. Anderson; Brian M. Dattilo; Paul M. Dunman; Russell Gerads; Richard M. Caprioli; Wolfgang Nacken; Walter Chazin; Eric P. Skaar

doi:10.1126/science.1152449

Metal Chelation and Inhibition of Bacterial Growth in Tissue Abscesses

Brian D. Corbin(Augenstern), Erin H. Seeley(Augenstern), Andrea Raab(Augenstern), Jörg Feldmann(Augenstern), Michael R. Miller(Augenstern), Victor J. Torres(Augenstern), Kelsi L. Anderson(Augenstern), Brian M. Dattilo(Augenstern), Paul M. Dunman(Augenstern), Russell Gerads(Augenstern), Richard M. Caprioli(Augenstern), Wolfgang Nacken(Augenstern), Walter Chazin(Augenstern), Eric P. Skaar(Augenstern)

Science

February 14, 2008

10.1126/science.1152449

Cited by 853

Abstract

Bacterial infection often results in the formation of tissue abscesses, which represent the primary site of interaction between invading bacteria and the innate immune system. We identify the host protein calprotectin as a neutrophil-dependent factor expressed inside Staphylococcus aureus abscesses. Neutrophil-derived calprotectin inhibited S. aureus growth through chelation of nutrient Mn2+ and Zn2+: an activity that results in reprogramming of the bacterial transcriptome. The abscesses of mice lacking calprotectin were enriched in metal, and staphylococcal proliferation was enhanced in these metal-rich abscesses. These results demonstrate that calprotectin is a critical factor in the innate immune response to infection and define metal chelation as a strategy for inhibiting microbial growth inside abscessed tissue.

Related Papers

No related papers found

Powered by citation graph analysis