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A proliferative to invasive switch is mediated by srGAP1 downregulation through the activation of TGF-β2 signaling

Many breast cancer (BC) patients suffer from complications of metastatic disease. To form metastases, cancer cells must become migratory and coordinate both invasive and proliferative programs at distant organs. Here, we identify srGAP1 as a regulator of a proliferative-to-invasive switch in BC cell...

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Autores principales: Mondal, Chandrani, Gacha-Garay, Majo J., Larkin, Kathryn A., Adikes, Rebecca C., Di Martino, Julie S., Chien, Chen-Chi, Fraser, Madison, Eni-aganga, Ireti, Agullo-Pascual, Esperanza, Cialowicz, Katarzyna, Ozbek, Umut, Naba, Alexandra, Gaitas, Angelo, Fu, Tian-Ming, Upadhyayula, Srigokul, Betzig, Eric, Matus, David Q., Martin, Benjamin L., Bravo-Cordero, Jose Javier
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9596226/
https://www.ncbi.nlm.nih.gov/pubmed/36130489
http://dx.doi.org/10.1016/j.celrep.2022.111358
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author Mondal, Chandrani
Gacha-Garay, Majo J.
Larkin, Kathryn A.
Adikes, Rebecca C.
Di Martino, Julie S.
Chien, Chen-Chi
Fraser, Madison
Eni-aganga, Ireti
Agullo-Pascual, Esperanza
Cialowicz, Katarzyna
Ozbek, Umut
Naba, Alexandra
Gaitas, Angelo
Fu, Tian-Ming
Upadhyayula, Srigokul
Betzig, Eric
Matus, David Q.
Martin, Benjamin L.
Bravo-Cordero, Jose Javier
author_facet Mondal, Chandrani
Gacha-Garay, Majo J.
Larkin, Kathryn A.
Adikes, Rebecca C.
Di Martino, Julie S.
Chien, Chen-Chi
Fraser, Madison
Eni-aganga, Ireti
Agullo-Pascual, Esperanza
Cialowicz, Katarzyna
Ozbek, Umut
Naba, Alexandra
Gaitas, Angelo
Fu, Tian-Ming
Upadhyayula, Srigokul
Betzig, Eric
Matus, David Q.
Martin, Benjamin L.
Bravo-Cordero, Jose Javier
author_sort Mondal, Chandrani
collection PubMed
description Many breast cancer (BC) patients suffer from complications of metastatic disease. To form metastases, cancer cells must become migratory and coordinate both invasive and proliferative programs at distant organs. Here, we identify srGAP1 as a regulator of a proliferative-to-invasive switch in BC cells. High-resolution light-sheet microscopy demonstrates that BC cells can form actin-rich protrusions during extravasation. srGA-P1(low) cells display a motile and invasive phenotype that facilitates their extravasation from blood vessels, as shown in zebrafish and mouse models, while attenuating tumor growth. Interestingly, a population of srGAP1(low) cells remain as solitary disseminated tumor cells in the lungs of mice bearing BC tumors. Overall, srGAP1(low) cells have increased Smad2 activation and TGF-β2 secretion, resulting in increased invasion and p27 levels to sustain quiescence. These findings identify srGAP1 as a mediator of a proliferative to invasive phenotypic switch in BC cells in vivo through a TGF-β2-mediated signaling axis.
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spelling pubmed-95962262022-10-25 A proliferative to invasive switch is mediated by srGAP1 downregulation through the activation of TGF-β2 signaling Mondal, Chandrani Gacha-Garay, Majo J. Larkin, Kathryn A. Adikes, Rebecca C. Di Martino, Julie S. Chien, Chen-Chi Fraser, Madison Eni-aganga, Ireti Agullo-Pascual, Esperanza Cialowicz, Katarzyna Ozbek, Umut Naba, Alexandra Gaitas, Angelo Fu, Tian-Ming Upadhyayula, Srigokul Betzig, Eric Matus, David Q. Martin, Benjamin L. Bravo-Cordero, Jose Javier Cell Rep Article Many breast cancer (BC) patients suffer from complications of metastatic disease. To form metastases, cancer cells must become migratory and coordinate both invasive and proliferative programs at distant organs. Here, we identify srGAP1 as a regulator of a proliferative-to-invasive switch in BC cells. High-resolution light-sheet microscopy demonstrates that BC cells can form actin-rich protrusions during extravasation. srGA-P1(low) cells display a motile and invasive phenotype that facilitates their extravasation from blood vessels, as shown in zebrafish and mouse models, while attenuating tumor growth. Interestingly, a population of srGAP1(low) cells remain as solitary disseminated tumor cells in the lungs of mice bearing BC tumors. Overall, srGAP1(low) cells have increased Smad2 activation and TGF-β2 secretion, resulting in increased invasion and p27 levels to sustain quiescence. These findings identify srGAP1 as a mediator of a proliferative to invasive phenotypic switch in BC cells in vivo through a TGF-β2-mediated signaling axis. 2022-09-20 /pmc/articles/PMC9596226/ /pubmed/36130489 http://dx.doi.org/10.1016/j.celrep.2022.111358 Text en https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/ (https://creativecommons.org/licenses/by-nc-nd/4.0/) ).
spellingShingle Article
Mondal, Chandrani
Gacha-Garay, Majo J.
Larkin, Kathryn A.
Adikes, Rebecca C.
Di Martino, Julie S.
Chien, Chen-Chi
Fraser, Madison
Eni-aganga, Ireti
Agullo-Pascual, Esperanza
Cialowicz, Katarzyna
Ozbek, Umut
Naba, Alexandra
Gaitas, Angelo
Fu, Tian-Ming
Upadhyayula, Srigokul
Betzig, Eric
Matus, David Q.
Martin, Benjamin L.
Bravo-Cordero, Jose Javier
A proliferative to invasive switch is mediated by srGAP1 downregulation through the activation of TGF-β2 signaling
title A proliferative to invasive switch is mediated by srGAP1 downregulation through the activation of TGF-β2 signaling
title_full A proliferative to invasive switch is mediated by srGAP1 downregulation through the activation of TGF-β2 signaling
title_fullStr A proliferative to invasive switch is mediated by srGAP1 downregulation through the activation of TGF-β2 signaling
title_full_unstemmed A proliferative to invasive switch is mediated by srGAP1 downregulation through the activation of TGF-β2 signaling
title_short A proliferative to invasive switch is mediated by srGAP1 downregulation through the activation of TGF-β2 signaling
title_sort proliferative to invasive switch is mediated by srgap1 downregulation through the activation of tgf-β2 signaling
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9596226/
https://www.ncbi.nlm.nih.gov/pubmed/36130489
http://dx.doi.org/10.1016/j.celrep.2022.111358
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