Intercellular adhesion molecule-1 (ICAM-1) is expressed on a variety of cells including endothelial cells, alveolar epithelial cells, and alveolar macrophages. Endothelial/epithelial cell ICAM-1 participates in the migration of leukocytes out of the blood in response to pulmonary inflammation, whereas alveolar macrophage ICAM-1 may represent cell activation. Our previous studies have shown that there is increased expression of ICAM-1 in lung tissue during acute inflammation following intratracheal injection with silica particles (2 mg/mouse). This increased expression was shown to play a role, in part, in the migration of neutrophils from the circulation into the tissue parenchyma. The aim of the current work is to localize expression of ICAM-1 during acute inflammation in lungs of mice exposed to either silica or the nuisance dust, titanium dioxide. In silica-exposed mice, a significant increase in ICAM-1 was detected on day 1 and localized by immunohistochemistry to aggregates of pulmonary macrophages and to type ii epithelial cells. Areas of the lung with increased ICAM-1 expression also showed increased tumor necrosis factor alpha expression. Immunocytochemical staining of bronchoalveolar lavage (BAL) cells demonstrated increased ICAM-1 expression associated with alveolar macrophages 3, 5, and 7 days following silica exposure. Finally, soluble ICAM-1 levels in the BAL fluid were significantly increased in mice exposed to silica on the same days. Titanium dioxide exposure elicited a minimal increase in expression of ICAM-1 in the lungs. These data demonstrate that exposure to the toxic particle silica specifically increases ICAM-1 expression localized to pulmonary macrophages and type ii epithelial cells.
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CHANG GUNG MEM HOSP,DEPT SURG PATHOL & DIAGNOST RADIOL,DIV GEN SURG,CHANG GUNG MED COLL,KAOHSIUNGHSIEN,TAIWANCHANG GUNG MEM HOSP,DEPT SURG PATHOL & DIAGNOST RADIOL,DIV GEN SURG,CHANG GUNG MED COLL,KAOHSIUNGHSIEN,TAIWAN
SheenChen, SM
Eng, HL
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CHANG GUNG MEM HOSP,DEPT SURG PATHOL & DIAGNOST RADIOL,DIV GEN SURG,CHANG GUNG MED COLL,KAOHSIUNGHSIEN,TAIWANCHANG GUNG MEM HOSP,DEPT SURG PATHOL & DIAGNOST RADIOL,DIV GEN SURG,CHANG GUNG MED COLL,KAOHSIUNGHSIEN,TAIWAN
Eng, HL
Cheng, YF
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CHANG GUNG MEM HOSP,DEPT SURG PATHOL & DIAGNOST RADIOL,DIV GEN SURG,CHANG GUNG MED COLL,KAOHSIUNGHSIEN,TAIWANCHANG GUNG MEM HOSP,DEPT SURG PATHOL & DIAGNOST RADIOL,DIV GEN SURG,CHANG GUNG MED COLL,KAOHSIUNGHSIEN,TAIWAN
Cheng, YF
Chou, FF
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CHANG GUNG MEM HOSP,DEPT SURG PATHOL & DIAGNOST RADIOL,DIV GEN SURG,CHANG GUNG MED COLL,KAOHSIUNGHSIEN,TAIWANCHANG GUNG MEM HOSP,DEPT SURG PATHOL & DIAGNOST RADIOL,DIV GEN SURG,CHANG GUNG MED COLL,KAOHSIUNGHSIEN,TAIWAN
Chou, FF
Chen, WJ
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CHANG GUNG MEM HOSP,DEPT SURG PATHOL & DIAGNOST RADIOL,DIV GEN SURG,CHANG GUNG MED COLL,KAOHSIUNGHSIEN,TAIWANCHANG GUNG MEM HOSP,DEPT SURG PATHOL & DIAGNOST RADIOL,DIV GEN SURG,CHANG GUNG MED COLL,KAOHSIUNGHSIEN,TAIWAN