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Early host cell targets of Yersinia pestis during primary pneumonic plague.

ABSTRACT: Inhalation of Yersinia pestis causes primary pneumonic plague, a highly lethal syndrome with mortality rates approaching 100%. Pneumonic plague progression is biphasic, with an initial pre-inflammatory phase facilitating bacterial growth in the absence of host inflammation, followed by a pro-inflammatory phase marked by extensive neutrophil influx, an inflammatory cytokine storm, and severe tissue destruction. Using a FRET-based probe to quantitate injection of effector proteins by the Y. pestis type III secretion system, we show that these bacteria target alveolar macrophages early during infection of mice, followed by a switch in host cell preference to neutrophils. We also demonstrate that neutrophil influx is unable to limit bacterial growth in the lung and is ultimately responsible for the severe inflammation during the lethal pro-inflammatory phase.

SUBMITTER: Pechous RD 

PROVIDER: S-EPMC3789773 | biostudies-literature | 2013

REPOSITORIES: biostudies-literature

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Early host cell targets of Yersinia pestis during primary pneumonic plague.

Pechous Roger D RD   Sivaraman Vijay V   Price Paul A PA   Stasulli Nikolas M NM   Goldman William E WE  

PLoS pathogens 20131003 10

Inhalation of Yersinia pestis causes primary pneumonic plague, a highly lethal syndrome with mortality rates approaching 100%. Pneumonic plague progression is biphasic, with an initial pre-inflammatory phase facilitating bacterial growth in the absence of host inflammation, followed by a pro-inflammatory phase marked by extensive neutrophil influx, an inflammatory cytokine storm, and severe tissue destruction. Using a FRET-based probe to quantitate injection of effector proteins by the Y. pestis  ...[more]

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