Journal
SCIENCE
Volume 358, Issue 6367, Pages 1202-+Publisher
AMER ASSOC ADVANCEMENT SCIENCE
DOI: 10.1126/science.aam8897
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Funding
- German Research Society [KFO 306, FU 742/4-1, SFB 841, INST 152/621-1, SFB 877, INST 257/433-1, SFB 1192, INST 152/692-1, INST 152/686-1]
- Stiftung fur Pathobiochemie und Molekulare Diagnostik of the German Society for Clinical Chemistry and Laboratory Medicine
- FoRUM-program of the Ruhr-University Bochum [F505-2006]
- Hjart Lungfonden [20110500]
- Vetenskapsradet [K2013-65X-21462-04-5]
- European Research Council [ERC-StG-2012-311575_F-12, PIIF-GA-2013-628264]
- Ardea Biosciences, Inc.
- Grants-in-Aid for Scientific Research [17K08891] Funding Source: KAKEN
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Platelet and fibrin clots occlude blood vessels in hemostasis and thrombosis. Here we report a noncanonical mechanism for vascular occlusion based on neutrophil extracellular traps (NETs), DNA fibers released by neutrophils during inflammation. We investigated which host factors control NETs in vivo and found that two deoxyribonucleases (DNases), DNase1 and DNase1-like 3, degraded NETs in circulation during sterile neutrophilia and septicemia. In the absence of both DNases, intravascular NETs formed clots that obstructed blood vessels and caused organ damage. Vascular occlusions in patients with severe bacterial infections were associated with a defect to degrade NETs ex vivo and the formation of intravascular NET clots. DNase1 and DNase1-like 3 are independently expressed and thus provide dual host protection against deleterious effects of intravascular NETs.
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