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Ambient particulate matter accelerates coagulation via an IL-6–dependent pathway
Gökhan M. Mutlu, … , Jacob I. Sznajder, G.R. Scott Budinger
Gökhan M. Mutlu, … , Jacob I. Sznajder, G.R. Scott Budinger
Published October 1, 2007
Citation Information: J Clin Invest. 2007;117(10):2952-2961. https://doi.org/10.1172/JCI30639.
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Research Article Cardiology

Ambient particulate matter accelerates coagulation via an IL-6–dependent pathway

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Abstract

The mechanisms by which exposure to particulate matter increases the risk of cardiovascular events are not known. Recent human and animal data suggest that particulate matter may induce alterations in hemostatic factors. In this study we determined the mechanisms by which particulate matter might accelerate thrombosis. We found that mice treated with a dose of well characterized particulate matter of less than 10 μM in diameter exhibited a shortened bleeding time, decreased prothrombin and partial thromboplastin times (decreased plasma clotting times), increased levels of fibrinogen, and increased activity of factor II, VIII, and X. This prothrombotic tendency was associated with increased generation of intravascular thrombin, an acceleration of arterial thrombosis, and an increase in bronchoalveolar fluid concentration of the prothrombotic cytokine IL-6. Knockout mice lacking IL-6 were protected against particulate matter–induced intravascular thrombin formation and the acceleration of arterial thrombosis. Depletion of macrophages by the intratracheal administration of liposomal clodronate attenuated particulate matter–induced IL-6 production and the resultant prothrombotic tendency. Our findings suggest that exposure to particulate matter triggers IL-6 production by alveolar macrophages, resulting in reduced clotting times, intravascular thrombin formation, and accelerated arterial thrombosis. These results provide a potential mechanism linking ambient particulate matter exposure and thrombotic events.

Authors

Gökhan M. Mutlu, David Green, Amy Bellmeyer, Christina M. Baker, Zach Burgess, Nalini Rajamannan, John W. Christman, Nancy Foiles, David W. Kamp, Andrew J. Ghio, Navdeep S. Chandel, David A. Dean, Jacob I. Sznajder, G.R. Scott Budinger

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Figure 1

Alterations in hemostasis in wild-type mice treated with PM.

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Alterations in hemostasis in wild-type mice treated with PM.
Airborne PM...
Airborne PM10 (10 μg in 50 μl PBS) or PBS alone was intratracheally instilled into mouse lungs, and 24 hours later measurements of hemostasis were made. (A) Bleeding time, platelet count, PT, and aPTT measurements. (B) Fibrinogen and coagulation factors (factors II, V, VII, VIII, and X). The number inside each bar represents the number of animals for each group of experiments. *P < 0.05 for comparison between PM- and PBS-treated mice, n ≥ 8 in each treatment group.

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