LTB4 is present in exudative pleural effusions and contributes actively to neutrophil recruitment in the inflamed pleural space

6533b859fe1ef96bd12b6fac

RESEARCH PRODUCT

LTB4 is present in exudative pleural effusions and contributes actively to neutrophil recruitment in the inflamed pleural space

Giovanni Bonsignore Mirella Profita Maria Ferraro Enrico Pace Mario Spatafora Antonio M. Vignola Mario Melis Alessandra Paternò Anna Bonanno Liboria Siena Christopher H. Mody Mark Gjomarkaj

subject

Lipopolysaccharides Pathology Hot Temperature Neutrophils Leukotriene B4 Gene Expression Epithelium chemistry.chemical_compound Neoplasms Clinical Studies Immunology and Allergy Medicine Respiratory system Pancreatic Elastase biology Neutrophil Middle Aged respiratory system Chemotaxis Leukocyte medicine.anatomical_structure Neutrophil Infiltration Neutrophil elastase LTB4 Pleura lipids (amino acids peptides and proteins)medicine.symptom Adult medicine.medical_specialty Immunology Inflammation Granulocyte Leukotriene B4 Humans RNA Messenger Tuberculosis Pulmonary Aged Arachidonate 5-Lipoxygenase Lung business.industry Pneumonia Macrophage Activation medicine.disease respiratory tract diseases Pleural Effusion Pneumonia Eicosanoid chemistry Immunology biology.protein business

description

SUMMARY The pleural space is a virtual compartment between the lung and chest wall that becomes filled with fluid and inflammatory cells during a variety of respiratory diseases. Here, we study the potential role of the eicosanoid metabolite leukotriene B4 (LTB4) in disparate diseases leading to acute (pneumonia) or chronic (tuberculosis, cancer) inflammation of the pleural space. LTB4 concentrations were significantly higher in pleural fluid due to pneumonia, tuberculosis and cancer with respect to congestive heart failure and correlated with neutrophil elastase, which is used as an indication of state of activation of neutrophils in the pleural space. Moreover, pleural LTB4 was biologically active, as an anti-LTB4 antibody partially neutralized the chemotactic activity of parapneumonic, tuberculous and cancer effusions. Macrophages, neutrophils, lymphocytes, mesothelial cells and cancer cells all expressed mRNA for 5-lipoxygenase, the enzyme that initiates leukotriene synthesis leading to the production of LTB4, in exudative pleural effusions. Upon stimulation in transudative pleural effusions, pleural macrophages produced, in a time-dependent fashion, a significantly higher concentration of LTB4 than mesothelial cells. These studies demonstrate that different cell types are capable of producing LTB4 in the inflamed pleural space and that this mediator may play a crucial role in the recruitment of neutrophils into the pleural space.

year	journal	country	edition	language
2004-03-11	Clinical and Experimental Immunology

https://doi.org/10.1111/j.1365-2249.2003.02387.x