Mononuclear Cells in Exudative Malignant Pleural Effusions: Characterization of Pleural Phagocytic Cells

doi:10.1378/chest.106.4.1042

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Mononuclear Cells in Exudative Malignant Pleural Effusions

Characterization of Pleural Phagocytic Cells

Mark Gjomarkaj M.D.¹; Elisabetta Pace M.D.¹; Mario Melis M.D.¹; Mario Spatafora M.D., F.C.C.P.²; and Galen B. Toews M.D.³

¹ From the Istituto di Fisiopatologia Respiratoria, Consiglio Nazionale delle Ricerche, Palermo, Italy
² From the Istituto di Medicina Generale e Pneumologia, Università degli Studi, Palermo, Italy
³ From the Division of Pulmonary and Critical Care Medicine, Department of Internal Medicine, University of Michigan, Ann Arbor

The aims of this study were to develop a methodology for theisolation of highly enriched mononuclear phagocyte populationsfrom exudative malignant pleural effusions (EMPE) and to characterizethe phenotype and functional properties of these cells. Pleuraleffusion mononuclear cells (PEMC) were isolated by Ficoll centrifugationof EMPE and transudative pleural effusions and allowed to adhereto plastic for 1 h to obtain pleural effusion mononuclear adherentcell (PEMAC) fraction. Only 66.0±4.2 percent of PEMAC ingestedlatex particles, indicating that a significant proportion ofPEMAC were not phagocytic cells. Latex-positive PEMAC had themorphologic appearance of macrophages and stained positive (97.3± 4.3 percent) with the anti-CD68 monoclonal antibody (MoAb),specific for macrophages. Conversely, latex-negative PEMAC (34.0± 4.1 percent of PEMAC) did not react with the anti- CD68MoAb and stained with anti-CD3 (34.7 ± 10.7 percent) andanticytokeratin (50.5 ± 16.4 percent) Mo- Abs, indicatingthat T cells and mesothelial cells were present in the PEMACfraction. To improve the purification of pleural macrophages,PEMAC were cultured for an additional 18 h and the cells thatremained adherent after this period constituted the firmly adherentmononuclear cell (FAMC) fraction. Nearly 90 percent of FAMCingested latex particles and were CD68- positive. Virtuallyall FAMC were CD3-negative and cytokeratin-negative. Similarpercentages of FAMC from EMPE and transudative effusions expressedthe monocyte-lineage markers CD1lb and CD14, suggesting thatthe proportion of monocyte-like mononuclear phagocytes in thepleural space is not increased during local tumor-associatedinflammatory responses. The FAMC from EMPE (1) expressed HLA-DRantigens, (2) released interleukin 1 (IL-1) β, and tumornecrosis factor (TNF) $agr$ , and (3) stimulated allogeneic T-lymphocyteproliferation. The results of this study suggest that pleuralmononuclear phagocytes may be involved in tumor-associated inflammatoryreactions in the pleural compartment by stimulating the proliferationof other inflammatory cells and by releasing inflammatory cytokines.

Key Words: mononuclear phagocytes • macrophages • pleura • pleural effusion • accessory cells • pleural macrophages

Submitted on March 16, 1993
Accepted on February 3, 1994

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