Diesel Exhaust Particles in Lung Acutely Enhance Experimental Peripheral Thrombosis

Nemmar, Abderrahim; Hoet, Peter; Dinsdale, David; Vermylen, Jozef; Hoylaerts, Marc; Nemery, Benoît

doi:10.1161/01.cir.0000053568.13058.67

Cited by 255 publications

(268 citation statements)

References 42 publications

(60 reference statements)

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“…Alternatively, the middle-aged population in epidemiological studies, though free of known cardiovascular disease, may have had some subclinical disease making them relatively more prone to inflammation than our young population. We also did not find a DE-associated increase in platelet numbers, consistent with prior study in a hamster model of DE particle exposure [20]. However, we did not directly test platelet activation, a more sensitive measure for which there is evidence in this hamster model.…”

Section: Discussionsupporting

confidence: 88%

Coagulation markers in healthy human subjects exposed to diesel exhaust

Carlsten

Kaufman

Peretz

et al. 2007

Thrombosis Research

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Background-Ambient particulate matter (PM) is associated with cardiovascular morbidity and mortality. It has been proposed that PM induces a pro-thrombotic process, increasing the risk of cardiovascular events, with some support from epidemiological and laboratory-based models. Diesel exhaust is a major contributor to urban PM, and we conducted a controlled human exposure of diesel exhaust in healthy subjects.

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Section: Discussionsupporting

confidence: 88%

Coagulation markers in healthy human subjects exposed to diesel exhaust

Carlsten

Kaufman

Peretz

et al. 2007

Thrombosis Research

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“…Studies from several laboratories including our own (15, 19, 32, 48 -50) have demonstrated that a systemic inflammatory response is induced by exposure to ambient particulate matter exposure, supporting the hypothesis put forward by Seaton and colleagues (41). This systemic response is characterized by an increased release of PMN (49) and monocytes (19) from the bone marrow as well as elevated levels of circulating cytokines such as IL-6 and IL-1␤ (48), CRP (36), and procoagulation factors (15,32). Elevated levels of these proinflammatory effector cells and mediators in the circulation have been implicated in the pathogenesis of progression and destabilization Fig.…”

Section: Discussionsupporting

confidence: 72%

“…Recently several studies have shown that ultrafine particulate matter (UFP) can translocate from the lung into the peripheral blood (32)(33)(34); the biological downstream effects on circulating blood cells and blood vessels are still unclear. We speculate that translocated UFP may contribute to the decrease in circulating monocytes expressing CD11b after PM 10 exposure.…”

Section: Discussionmentioning

confidence: 99%

Particulate matter air pollution exposure promotes recruitment of monocytes into atherosclerotic plaques

Yatera

Hsieh²,

Hogg³

et al. 2008

American Journal of Physiology-Heart and Circulatory Physiology

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demiologic studies have shown an association between exposure to ambient particulate air pollution Ͻ10 m in diameter (PM10) and increased cardiovascular morbidity and mortality. We previously showed that PM10 exposure causes progression of atherosclerosis in coronary arteries. We postulate that the recruitment of monocytes from the circulation into atherosclerotic lesions is a key step in this PM10-induced acceleration of atherosclerosis. The study objective was to quantify the recruitment of circulating monocytes into vessel walls and the progression of atherosclerotic plaques induced by exposure to PM10. Female Watanabe heritable hyperlipidemic rabbits, which naturally develop systemic atherosclerosis, were exposed to PM10 (EHC-93) or vehicle by intratracheal instillation twice a week for 4 wk. Monocytes, labeled with 5-bromo-2Ј-deoxyuridine (BrdU) in donors, were transfused to recipient rabbits as whole blood, and the recruitment of BrdU-labeled cells into vessel walls and plaques in recipients was measured by quantitative histological methodology. Exposure to PM10 caused progression of atherosclerotic lesions in thoracic and abdominal aorta. It also decreased circulating monocyte counts, decreased circulating monocytes expressing high levels of CD31 (platelet endothelial cell adhesion molecule-1) and CD49d (very late antigen-4 ␣-chain), and increased expression of CD54 (ICAM-1) and CD106 (VCAM-1) in plaques. Exposure to PM10 increased the number of BrdU-labeled monocytes adherent to endothelium over plaques and increased the migration of BrdU-labeled monocytes into plaques and smooth muscle underneath plaques. We conclude that exposure to ambient air pollution particles promotes the recruitment of circulating monocytes into atherosclerotic plaques and speculate that this is a critically important step in the PM10-induced progression of atherosclerosis. atherosclerosis; adhesion molecules EPIDEMIOLOGIC STUDIES have associated exposure to ambient particulate air pollution Ͻ10 m in diameter (PM 10

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“…In addition, morphological study showed instilled 30 nm gold particles in capillaries within 30 minutes' postexposure (Berry et al, 1977) and inhaled ultrafine titanium dioxide particles at alveolar wall and in capillaries at 1 hour after the end of exposure (Geiser et al, 2005). UFPs in the blood circulation can directly or indirectly influence hemostasis or cardiovascular integrity and thus induce adverse cardiovascular endpoints more directly (Nemmar et al, 2002b(Nemmar et al, , 2003a(Nemmar et al, , 2003b. The exact pathway for this translocation, however, remains unclear.…”

Section: Introductionmentioning

confidence: 99%

Translocation Pathway of the Intratracheally Instilled Ultrafine Particles from the Lung into the Blood Circulation in the Mouse

et al. 2006

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Recently, it has been demonstrated that ultrafine particles (UFPs) are able to translocate from the lung into the systemic circulation. Precise mechanisms of the anatomical translocation (crossing the air-blood barrier) of inhaled UFPs at the alveolar wall are not fully understood. In this study, we examined the translocation pathway of the intratracheally instilled ultrafine carbon black (UFCB) from the lung into the blood circulation in mouse. Electron microscopy demonstrated accumulation of intratracheally instilled UFCB in the large-sized gaps developing between the cytoplasmic processes of the alveolar epithelial cells, possibly as a result of shrinkage of cytoplasm, by receiving stimulus/signals generated and released following UFCB attachment on the alveolar epithelial cells. Occasional penetration of the accumulated UFCB into the alveolar basement membrane, exposing to the air space, was observed at the gap. These results suggest that inhaled UFPs may, in part, pass the air-blood barrier through the large-sized gap formed between the alveolar epithelial cells.

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Diesel Exhaust Particles in Lung Acutely Enhance Experimental Peripheral Thrombosis

Cited by 255 publications

References 42 publications

Coagulation markers in healthy human subjects exposed to diesel exhaust

Coagulation markers in healthy human subjects exposed to diesel exhaust

Particulate matter air pollution exposure promotes recruitment of monocytes into atherosclerotic plaques

Translocation Pathway of the Intratracheally Instilled Ultrafine Particles from the Lung into the Blood Circulation in the Mouse

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