Desmoid tumor-associated pain is dependent on mast cell expression of cyclooxygenase-2

Desmoid tumors are rare clonal fibroblastic proliferations that arise in the extremities, girdles, chest, abdominal wall, and neck. They are characterized by infiltrative growth and a high risk of local recurrence even after complete surgical excision[1]. Several reports have suggested a link between cyclooxygenase-2 (COX-2) expression and the proliferation of desmoid tumors[2, 3]. These findings provide clinical evidence for the use of COX-2 inhibitors in the treatment of desmoid tumors. Most patients present with an asymptomatic, firm, poorly circumscribed mass, but some complain of severe tumor-associated pain. These painful masses often cause decreased joint mobility and functional impairment. COX-2 converts arachidonic acid into prostaglandins, the major modulator of pain. In this study, the hypothesis that COX-2 regulates desmoid tumor-associated pain was examined by immunohistochemical evaluation of COX-2 expression in tumor samples. The relationship between intratumoral COX-2 expression and pain status was evaluated.

For the use of these clinical materials for research purposes, prior consent from the patients and approval from the Institutional Review Board of Sapporo Medical University Hospital was obtained.

Mast cells are mobile cells derived from bone marrow that circulate in the blood. Mature mast cells are scattered throughout tissues, including connective tissue[4]. The role of mast cells in connective tissue is still a matter of speculation, and it has been suggested that these cells participate in cell regulation and control of the accumulation of connective tissue components. Several reports indicate that mast cells are potentially fibrogenic, since they secrete potent mediators of fibrosis[5, 6]. One of the main components of the secretory granules of mast cells is tryptase[7], an enzyme found exclusively in these cells. Tryptase is involved in diverse biological activities such as fibrogenesis and stimulation of fibroblast proliferation[8, 9]. These findings suggest that mast cells are involved in the pathogenesis of desmoid tumors through the action of tryptase, a mast cell-derived protease. Recent studies have shown that tryptase induces COX-2 expression by the specific cleavage of protease-activated receptor-2[10, 11]. COX-2 expression is significantly elevated in several neoplasms, including desmoids tumor[2, 3]. COX-2 overexpression leads to increased prostaglandin E2 production, which in turn promotes the growth of desmoid tumors. Furthermore, treatment with COX-2 inhibitors induces the shrinkage of desmoid tumors.

Recent reports have demonstrated that desmoids tumor cells express COX-2 protein[2, 3]. However, we failed to show the expression of COX-2 protein within the tumor cells. Conversely, COX-2 -positive mast cells were identified within the desmoid tumors. In addition, a positive correlation between COX-2 expression and tumor-related pain was observed, suggesting that COX-2 secretion from mast cells, not tumor cells, may modulate desmoid tumor-related pain. In addition, there could be connection between mast cells, at least in part, and the pathogenesis of desmoids tumors.

In conclusion, these results suggest a link between clinical symptoms and the tumor microenvironment in desmoid tumors via the secretion of COX-2 from mast cells.