Directed transport of neutrophil-derived extracellular vesicles enables platelet-mediated innate immune response

The innate immune response to bacterial infections requires the interaction of neutrophils and platelets. Here, we show that a multistep reciprocal crosstalk exists between these two cell types, ultimately facilitating neutrophil influx into the lung to eliminate infections. Activated platelets adhe...

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Vydané v:	Nature communications Ročník 7; číslo 1; s. 13464 - 14
Hlavní autori:	Rossaint, Jan, Kühne, Katharina, Skupski, Jennifer, Van Aken, Hugo, Looney, Mark R., Hidalgo, Andres, Zarbock, Alexander
Médium:	Journal Article
Jazyk:	English
Vydavateľské údaje:	London Nature Publishing Group UK 15.11.2016 Nature Publishing Group Nature Portfolio
Predmet:	13/1 13/31 14/19 14/63 631/250/2504/223/1699 631/443/592/1339 64/60 Acids Animals Bacterial diseases Bacterial infections Biological Transport - immunology Blood Platelets - immunology Blood Platelets - metabolism Cyclooxygenase 1 - genetics Cyclooxygenase 1 - immunology Cyclooxygenase 1 - metabolism Escherichia coli Infections - genetics Escherichia coli Infections - immunology Escherichia coli Infections - metabolism Extracellular vesicles Extracellular Vesicles - immunology Extracellular Vesicles - metabolism Glycoproteins Humanities and Social Sciences Immune response Immunity - immunology Male Membrane Glycoproteins - immunology Membrane Glycoproteins - metabolism Metabolism Metabolites Mice, Inbred C57BL Mice, Knockout multidisciplinary Neutrophils Neutrophils - immunology Neutrophils - metabolism P-Selectin - immunology P-Selectin - metabolism Platelet Adhesiveness - immunology Platelet Glycoprotein GPIb-IX Complex - immunology Platelet Glycoprotein GPIb-IX Complex - metabolism Pneumonia Pneumonia, Bacterial - genetics Pneumonia, Bacterial - immunology Pneumonia, Bacterial - metabolism Science Science (multidisciplinary) Thromboxane A2 - immunology Thromboxane A2 - metabolism United States > US Germany California
ISSN:	2041-1723, 2041-1723
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Shrnutí:	The innate immune response to bacterial infections requires the interaction of neutrophils and platelets. Here, we show that a multistep reciprocal crosstalk exists between these two cell types, ultimately facilitating neutrophil influx into the lung to eliminate infections. Activated platelets adhere to intravascular neutrophils through P-selectin/P-selectin glycoprotein ligand-1 (PSGL-1)-mediated binding, a primary interaction that allows platelets glycoprotein Ibα (GPIbα)-induced generation of neutrophil-derived extracellular vesicles (EV). EV production is directed by exocytosis and allows shuttling of arachidonic acid into platelets. EVs are then specifically internalized into platelets in a Mac1-dependent fashion, and relocated into intracellular compartments enriched in cyclooxygenase1 (Cox1), an enzyme processing arachidonic acid to synthesize thromboxane A 2 (TxA 2 ). Finally, platelet-derived-TxA 2 elicits a full neutrophil response by inducing the endothelial expression of ICAM-1, intravascular crawling, and extravasation. We conclude that critical substrate–enzyme pairs are compartmentalized in neutrophils and platelets during steady state limiting non-specific inflammation, but bacterial infection triggers regulated EV shuttling resulting in robust inflammation and pathogen clearance. Interaction between platelets and neutrophils promotes neutrophil activation. Here the authors show that neutrophils initiate the cross-talk with platelets by shuttling arachidonic acid via extracellular vesicles, which platelets convert to thromboxane A 2 that then elicits neutrophil activation.
Bibliografia:	ObjectType-Article-1 SourceType-Scholarly Journals-1 ObjectType-Feature-2 content type line 14 content type line 23
ISSN:	2041-1723 2041-1723
DOI:	10.1038/ncomms13464