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Giannou, A.D.* ; Marazioti, A.* ; Spella, M.* ; Kanellakis, N.I.* ; Apostolopoulou, H.* ; Psallidas, L.* ; Prijovich, Z.M.* ; Vreka, M.* ; Zazara, D.E.* ; Lilis, L.* ; Papaleonidopoulos, V.* ; Kairi, C.A.* ; Patmanidi, A.L.* ; Giopanou, J.* ; Spiropoulou, N.* ; Harokopos, V.* ; Aidinis, V.* ; Spyratos, D.* ; Teliousi, S.* ; Papadaki, H.* ; Taraviras, S.* ; Snyder, L.A.* ; Eickelberg, O. ; Kardamakis, D.* ; Iwakura, V.* ; Feyerabend, T.B.* ; Rodewald, H.R.* ; Kalomenidis, L.* ; Blackwell, T.S.* ; Agalloti, T.* ; Stathopoulos, G.T.

Mast cells mediate malignant pleural effusion formation.

J. Clin. Invest. 125, 2317-2334 (2015)

DOI

Open Access Gold möglich sobald Verlagsversion bei der ZB eingereicht worden ist.

Abstract
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Mast cells (MCs) have been identified in various tumors; however, the role of these cells in tumorigenesis remains controversial. Here, we quantified MCs in human and murine malignant pleural effusions (MPEs) and evaluated the fate and function of these cells in MPE development. Evaluation of murine MPE-competent lung and colon adenocarcinomas revealed that these tumors actively attract and subsequently degranulate MCs in the pleural space by elaborating CCL2 and osteopontin. MCs were required for effusion development, as MPEs did not form in mice lacking MCs, and pleural infusion of MCs with MPE-incompetent cells promoted MPE formation. Once homed to the pleural space, MCs released tryptase AB1 and IL-1 beta, which in turn induced pleural vasculature leakiness and triggered NF-kappa B activation in pleural tumor cells, thereby fostering pleural fluid accumulation and tumor growth. Evaluation of human effusions revealed that MCs are elevated in MPEs compared with benign effusions. Moreover, MC abundance correlated with MPE formation in a human cancer cell-induced effusion model. Treatment of mice with the c-KIT inhibitor imatinib mesylate limited effusion precipitation by mouse and human adenbcarcinoma cells. Together, the results of this study indicate that MCs are required for MPE formation and suggest that MC-dependent effusion formation is therapeutically addressable.

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Publikationstyp Artikel: Journalartikel

Dokumenttyp Wissenschaftlicher Artikel

Schlagwörter Factor-kappa-b; C-kit Gene; Lung Adenocarcinoma; Tumor Progression; Bone-marrow; Mouse Model; Stem-cells; Cancer; Mice; Inflammation

ISSN (print) / ISBN 0021-9738

e-ISSN 1558-8238

Zeitschrift Journal of Clinical Investigation

Quellenangaben Band: 125, Heft: 6, Seiten: 2317-2334

Verlag American Society of Clinical Investigation

Verlagsort Ann Arbor

Begutachtungsstatus Peer reviewed

Institut(e) Institute of Lung Health and Immunity (LHI)
German Center for Lung Research (DZL)