Mitochondrial damage-associated molecular patterns from fractures suppress pulmonary immune responses via formyl peptide receptors 1 and 2

Galenkamp, Amanda; Tang, I. Tien; Lee, Yen Ting; Zeng, Yi; Livingston, David H.; Li, Haipeng; Itagaki, Kiyoshi; Sandler, Nicola; Gallo, David; Kaczmarek, Elzbieta; Hauser, Carl J.; Otterbein, Leo; Isal, Burak

Tarih

2015

Yazar

Galenkamp, Amanda

Tang, I. Tien

Lee, Yen Ting

Zeng, Yi

Livingston, David H.

Li, Haipeng

Itagaki, Kiyoshi

Sandler, Nicola

Gallo, David

Kaczmarek, Elzbieta

Hauser, Carl J.

Otterbein, Leo

Isal, Burak

Üst veri

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Özet

BACKGROUND: No known biologic mechanisms link tissue injury with pneumonia (PNA). Neutrophils (PMNs) are innate immune cells that clear bacteria from the lung by migration toward chemoattractants and killing bacteria in neutrophil extracellular traps (NETs). We predicted that tissue injury would suppress PMN antimicrobial function in the lung. We have also shown that mitochondria-derived damage-associated molecular pattern molecules from the bone can alter PMN phenotype and so hypothesized that formyl peptides (FPs) from fractures predispose to PNA by suppressing PMN activity in the lung.

Bağlantı

http://hdl.handle.net/20.500.12627/41080
https://doi.org/10.1097/ta.0000000000000509

Koleksiyonlar

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