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Endoglin and MMP14 Contribute to Ewing Sarcoma Spreading by Modulation of Cell-Matrix Interactions

Authors :: European Commission
Instituto de Salud Carlos III
Centro de Investigación Biomédica en Red Cáncer (España)
Junta de Andalucía
Fundación CRIS contra el Cáncer
Asociación Candela Riera
Asociación Pablo Ugarte
Ministerio de Ciencia, Innovación y Universidades (España)
Agencia Estatal de Investigación (España)
Fundación María García Estrada
Universidad de Sevilla
Fundación Mari Paz Jiménez Casado
Grupo Español de Investigación en Sarcomas
Barbara and Wilfried Mohr Foundation
Todos somos Iván
Fundación LaSonrisaDeAlex
Puerto-Camacho, Pilar [0000-0001-5338-2610]
Díaz-Martín, J. [0000-0002-3985-6434]
Salguero-Aranda, Carmen0000-0001-6010-8302
Alamo-Alvarez, Inmaculada0000-0002-6295-0218
Delgado-Bellido, Daniel0000-0002-9588-4747
Dopazo, Joaquín0000-0003-3318-120X
Alonso, Javier0000-0002-6287-8391
Bernabéu, Carmelo0000-0002-1563-6162
Byron, Adam0000-0002-5939-9883
Brunton, Valerie G. 0000-0002-7778-8794
Álava, Enrique de [0000-0001-8400-046X]
Puerto-Camacho, Pilar
Díaz-Martín, J.
Olmedo-Pelayo, Joaquín
Bolado Carrancio, Alfonso
Salguero-Aranda, Carmen
Jordán-Pérez, Carmen
Esteban-Medina, Marina
Alamo-Alvarez, Inmaculada
Delgado-Bellido, Daniel
Lobo Selma, Laura
Dopazo, Joaquín
Sastre, Ana
Alonso, Javier
Grünewald, Thomas G. P.
Bernabéu, Carmelo
Byron, Adam
Brunton, Valerie G.
Amaral, Ana Teresa
Álava, Enrique de
European Commission
Instituto de Salud Carlos III
Centro de Investigación Biomédica en Red Cáncer (España)
Junta de Andalucía
Fundación CRIS contra el Cáncer
Asociación Candela Riera
Asociación Pablo Ugarte
Ministerio de Ciencia, Innovación y Universidades (España)
Agencia Estatal de Investigación (España)
Fundación María García Estrada
Universidad de Sevilla
Fundación Mari Paz Jiménez Casado
Grupo Español de Investigación en Sarcomas
Barbara and Wilfried Mohr Foundation
Todos somos Iván
Fundación LaSonrisaDeAlex
Puerto-Camacho, Pilar [0000-0001-5338-2610]
Díaz-Martín, J. [0000-0002-3985-6434]
Salguero-Aranda, Carmen0000-0001-6010-8302
Alamo-Alvarez, Inmaculada0000-0002-6295-0218
Delgado-Bellido, Daniel0000-0002-9588-4747
Dopazo, Joaquín0000-0003-3318-120X
Alonso, Javier0000-0002-6287-8391
Bernabéu, Carmelo0000-0002-1563-6162
Byron, Adam0000-0002-5939-9883
Brunton, Valerie G. 0000-0002-7778-8794
Álava, Enrique de [0000-0001-8400-046X]
Puerto-Camacho, Pilar
Díaz-Martín, J.
Olmedo-Pelayo, Joaquín
Bolado Carrancio, Alfonso
Salguero-Aranda, Carmen
Jordán-Pérez, Carmen
Esteban-Medina, Marina
Alamo-Alvarez, Inmaculada
Delgado-Bellido, Daniel
Lobo Selma, Laura
Dopazo, Joaquín
Sastre, Ana
Alonso, Javier
Grünewald, Thomas G. P.
Bernabéu, Carmelo
Byron, Adam
Brunton, Valerie G.
Amaral, Ana Teresa
Álava, Enrique de
Publication Year :: 2022
Abstract: Endoglin (ENG) is a mesenchymal stem cell (MSC) marker typically expressed by active endothelium. This transmembrane glycoprotein is shed by matrix metalloproteinase 14 (MMP14). Our previous work demonstrated potent preclinical activity of first-in-class anti-ENG antibody-drug conjugates as a nascent strategy to eradicate Ewing sarcoma (ES), a devastating rare bone/soft tissue cancer with a putative MSC origin. We also defined a correlation between ENG and MMP14 expression in ES. Herein, we show that ENG expression is significantly associated with a dismal prognosis in a large cohort of ES patients. Moreover, both ENG/MMP14 are frequently expressed in primary ES tumors and metastasis. To deepen in their functional relevance in ES, we conducted transcriptomic and proteomic profiling of in vitro ES models that unveiled a key role of ENG and MMP14 in cell mechano-transduction. Migration and adhesion assays confirmed that loss of ENG disrupts actin filament assembly and filopodia formation, with a concomitant effect on cell spreading. Furthermore, we observed that ENG regulates cell-matrix interaction through activation of focal adhesion signaling and protein kinase C expression. In turn, loss of MMP14 contributed to a more adhesive phenotype of ES cells by modulating the transcriptional extracellular matrix dynamics. Overall, these results suggest that ENG and MMP14 exert a significant role in mediating correct spreading machinery of ES cells, impacting the aggressiveness of the disease.

Details

Database :: OAIster
Notes :: English
Publication Type :: Electronic Resource
Accession number :: edsoai.on1380453392
Document Type :: Electronic Resource

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Endoglin and MMP14 Contribute to Ewing Sarcoma Spreading by Modulation of Cell-Matrix Interactions

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Endoglin and MMP14 Contribute to Ewing Sarcoma Spreading by Modulation of Cell-Matrix Interactions

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