OBJECTIVES We sought to determine the effect of exposure to air pollution particulate matter <10 mu m (PM10) on the progression of atherosclerosis in rabbits. BACKGROUND Epidemiologic studies have associated exposure to ambient PM10 with increased cardiovascular morbidity and mortality. We have previously shown that PM10 exposure induces a systemic inflammatory response that includes marrow stimulation, and we hypothesized that this response accelerates atherosclerosis. METHODS Watanabe heritable hyperlipidemic rabbits were exposed to PM10 (n = 10) or vehicle (n = 6) for four weeks, and bone marrow stimulation was measured. Quantitative histologic methods were used to determine the morphologic features of the atherosclerotic lesions. RESULTS Exposure to PM10 caused an increase in circulating polymorphonuclear leukocytes (PMN) band cell counts (day 15: 24.6 +/- 3.0 vs. 11.5 +/- 2.7 x 10(7)/1 [PM10 vs. vehicle], p < 0.01) and an increase in the size of the bone marrow mitotic pool of PMNs. Exposure to PM10 also caused progression of atherosclerotic lesions toward a more advanced phenotype. The volume fraction (vol/vol) of the coronary atherosclerotic lesions was increased by PM10 exposure (33.3 +/- 4.6% vs. 19.5 +/- 3.1% [PM10 vs. vehicle], p < 0.05). The vol/vol of atherosclerotic lesions correlated with the number of alveolar macrophages that phagocytosed PM,, (coronary arteries: r = 0.53, p < 0.05; aorta: r = 0.51, p < 0.05). Exposure to PM10 also caused an increase in plaque cell turnover and extracellular lipid pools in coronary and aortic lesions, as well as in the total amount of lipids in aortic lesions. CONCLUSIONS Progression of atherosclerosis and increased vulnerability to plaque rupture may underlie the relationship between particulate air pollution and excess cardiovascular death. (J Am Coll Cardiol 2002;39:935-42) (C) 2002 by the American College of Cardiology Foundation.
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Bascom R, 1996, AM J RESP CRIT CARE, V153, P3, DOI 10.1164/ajrccm.153.1.8542133
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UNIV BRITISH COLUMBIA,ST PAULS HOSP,PULM RES LAB,1081 BURRARD ST,VANCOUVER V6T 1Y6,BC,CANADAUNIV BRITISH COLUMBIA,ST PAULS HOSP,PULM RES LAB,1081 BURRARD ST,VANCOUVER V6T 1Y6,BC,CANADA
BICKNELL, S
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VANEEDEN, S
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UNIV BRITISH COLUMBIA,ST PAULS HOSP,PULM RES LAB,1081 BURRARD ST,VANCOUVER V6T 1Y6,BC,CANADAUNIV BRITISH COLUMBIA,ST PAULS HOSP,PULM RES LAB,1081 BURRARD ST,VANCOUVER V6T 1Y6,BC,CANADA
VANEEDEN, S
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HAYASHI, S
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UNIV BRITISH COLUMBIA,ST PAULS HOSP,PULM RES LAB,1081 BURRARD ST,VANCOUVER V6T 1Y6,BC,CANADAUNIV BRITISH COLUMBIA,ST PAULS HOSP,PULM RES LAB,1081 BURRARD ST,VANCOUVER V6T 1Y6,BC,CANADA
HAYASHI, S
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HARDS, J
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UNIV BRITISH COLUMBIA,ST PAULS HOSP,PULM RES LAB,1081 BURRARD ST,VANCOUVER V6T 1Y6,BC,CANADAUNIV BRITISH COLUMBIA,ST PAULS HOSP,PULM RES LAB,1081 BURRARD ST,VANCOUVER V6T 1Y6,BC,CANADA
HARDS, J
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ENGLISH, D
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UNIV BRITISH COLUMBIA,ST PAULS HOSP,PULM RES LAB,1081 BURRARD ST,VANCOUVER V6T 1Y6,BC,CANADAUNIV BRITISH COLUMBIA,ST PAULS HOSP,PULM RES LAB,1081 BURRARD ST,VANCOUVER V6T 1Y6,BC,CANADA
ENGLISH, D
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HOGG, JC
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UNIV BRITISH COLUMBIA,ST PAULS HOSP,PULM RES LAB,1081 BURRARD ST,VANCOUVER V6T 1Y6,BC,CANADAUNIV BRITISH COLUMBIA,ST PAULS HOSP,PULM RES LAB,1081 BURRARD ST,VANCOUVER V6T 1Y6,BC,CANADA
BICKNELL, S
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VANEEDEN, S
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UNIV BRITISH COLUMBIA,ST PAULS HOSP,PULM RES LAB,1081 BURRARD ST,VANCOUVER V6T 1Y6,BC,CANADAUNIV BRITISH COLUMBIA,ST PAULS HOSP,PULM RES LAB,1081 BURRARD ST,VANCOUVER V6T 1Y6,BC,CANADA
VANEEDEN, S
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HAYASHI, S
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UNIV BRITISH COLUMBIA,ST PAULS HOSP,PULM RES LAB,1081 BURRARD ST,VANCOUVER V6T 1Y6,BC,CANADAUNIV BRITISH COLUMBIA,ST PAULS HOSP,PULM RES LAB,1081 BURRARD ST,VANCOUVER V6T 1Y6,BC,CANADA
HAYASHI, S
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HARDS, J
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UNIV BRITISH COLUMBIA,ST PAULS HOSP,PULM RES LAB,1081 BURRARD ST,VANCOUVER V6T 1Y6,BC,CANADAUNIV BRITISH COLUMBIA,ST PAULS HOSP,PULM RES LAB,1081 BURRARD ST,VANCOUVER V6T 1Y6,BC,CANADA
HARDS, J
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ENGLISH, D
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HOGG, JC
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