Tenascin-C increases lung metastasis by impacting blood vessel invasions.
Zhen Sun, Inés Velázquez-Quesada, Devadarssen Murdamoothoo, Constance Ahowesso, Alev Yilmaz, Caroline Spenlé, Gerlinde Averous, William Erne, Felicitas Oberndorfer, Andre Oszwald, Renate Kain, Catherine Bourdon, Pierre Mangin, Claire Deligne, Kim Midwood, Chérine Abou-Faycal, Olivier Lefebvre, Annick Klein, Michael van der Heyden, Marie-Pierre Chenard, Gerhard Christofori, Carole Mathelin, Thomas Loustau, Thomas Hussenet, Gertraud Orend
Matrix biology : journal of the International Society for Matrix Biology 2019 OctMetastasis is a major cause of death in cancer patients. The extracellular matrix molecule tenascin-C is a known promoter of metastasis, however the underlying mechanisms are not well understood. To further analyze the impact of tenascin-C on cancer progression we generated MMTV-NeuNT mice that develop spontaneous mammary tumors, on a tenascin-C knockout background. We also developed a syngeneic orthotopic model in which tumor cells derived from a MMTV-NeuNT tumor. Tumor cells were transfected with control shRNA or with shRNA to knockdown tenascin-C expression and, were grafted into the mammary gland of immune competent, wildtype or tenascin-C knockout mice. We show that stromal-derived tenascin-C increases metastasis by reducing apoptosis and inducing the cellular plasticity of cancer cells located in pulmonary blood vessels invasions (BVI), before extravasation. We characterized BVI as organized structures of tightly packed aggregates of proliferating tumor cells with epithelial characteristics, surrounded by Fsp1+ cells, internally located platelets and, a luminal monolayer of endothelial cells. We found extracellular matrix, in particular, tenascin-C, between the stromal cells and the tumor cell cluster. In mice lacking stromal-derived tenascin-C, the organization of pulmonary BVI was significantly affected, revealing novel functions of host-derived tenascin-C in supporting the integrity of the endothelial cell coat, increasing platelet abundance, tumor cell survival, epithelial plasticity, thereby promoting overall lung metastasis. Many effects of tenascin-C observed in BVI including enhancement of cellular plasticity, survival and migration, could be explained by activation of TGF-β signaling. Finally, in several human cancers, we also observed BVI to be surrounded by an endothelial monolayer and to express tenascin-C. Expression of tenascin-C is specific to BVI and is not observed in lymphatic vascular invasions frequent in breast cancer, which lack an endothelial lining. Given that BVI have prognostic significance for many tumor types, such as shorter cancer patient survival, increased metastasis, vessel occlusion, and organ failure, our data revealing a novel mechanism by which stromal tenascin-C promotes metastasis in human cancer, may have potential for diagnosis and therapy. Copyright © 2019 The Authors. Published by Elsevier B.V. All rights reserved.
Citation
Zhen Sun, Inés Velázquez-Quesada, Devadarssen Murdamoothoo, Constance Ahowesso, Alev Yilmaz, Caroline Spenlé, Gerlinde Averous, William Erne, Felicitas Oberndorfer, Andre Oszwald, Renate Kain, Catherine Bourdon, Pierre Mangin, Claire Deligne, Kim Midwood, Chérine Abou-Faycal, Olivier Lefebvre, Annick Klein, Michael van der Heyden, Marie-Pierre Chenard, Gerhard Christofori, Carole Mathelin, Thomas Loustau, Thomas Hussenet, Gertraud Orend. Tenascin-C increases lung metastasis by impacting blood vessel invasions. Matrix biology : journal of the International Society for Matrix Biology. 2019 Oct;83:26-47
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PMID: 31288084
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