Crosstalk between the mesothelium and lymphomatous cells: insight into the mechanisms involved in the progression of body cavity lymphomas.

[primary effusion lymphoma]

The peculiar localization of body cavity lymphomas implies a specific contribution of the intracavitary microenvironment to the pathogenesis of these tumors . In this study , primary effusion lymphoma (PEL ) was used as a model of body cavity lymphoma to investigate the role of mesothelial cells , which line the serous cavities , in lymphoma progression . The crosstalk between mesothelial and lymphomatous cells was studied in cocultures of primary human mesothelial cells (HMC ) with PEL cells and a xenograft mouse model of peritoneal PEL . PEL cells were found to induce type 2 epithelial-mesenchymal transition (EMT ) in HMC , which converted into a myofibroblastic phenotype characterized by loss of epithelial markers (pan cytokeratin and E -cadherin ), expression of EMT-associated transcriptional repressors (Snail 1 , Slug , Zeb 1 , Sip 1 ), and acquisition of α-smooth muscle actin (α-SMA ), a mesenchymal protein . A progressive thickening of serosal membranes was observed in vivo , accompanied by loss of cytokeratin staining and appearance of α-SMA -expressing cells , confirming that fibrosis occurred during intracavitary PEL development . On the other hand , HMC were found to modulate PEL cell turnover in vitro , increasing their resistance to apoptosis and proliferation . This supportive activity on PEL cells was retained after transdifferentiation , and was impaired by interferon-α 2 b treatment . On the whole , our results indicate that PEL cells induce type 2 EMT in HMC , which support PEL cell growth and survival , providing a milieu favorable to lymphoma progression . Our findings provide new clues into the mechanisms involved in lymphoma progression and may indicate new targets for effective treatment of malignant effusions growing in body cavities .