Sequential combinations of chemotherapeutic agents with BH3 mimetics to treat rhabdomyosarcoma and avoid resistance

Clara Alcon; Albert Manzano-Muñoz; Estela Prada; Jaume Mora; Aroa Soriano; Gabriela Guillén; Soledad Gallego; Josep Roma; Josep Samitier; Alberto Villanueva; Joan Montero

doi:10.1038/s41419-020-02887-y

Sequential combinations of chemotherapeutic agents with BH3 mimetics to treat rhabdomyosarcoma and avoid resistance

Clara Alcon, Albert Manzano-Muñoz, Estela Prada, Jaume Mora, Aroa Soriano, Gabriela Guillén, Soledad Gallego, Josep Roma, Josep Samitier, Alberto Villanueva, Joan Montero

Departament de Pediatria, d’Obstetrícia i Ginecologia i de Medicina Preventiva i Salut Pública

Producció científica: Contribució a revista › Article › Recerca › Avaluat per experts

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Rhabdomyosarcoma (RMS) is the most common soft tissue sarcoma in childhood and adolescence. Refractory/relapsed RMS patients present a bad prognosis that combined with the lack of specific biomarkers impairs the development of new therapies. Here, we utilize dynamic BH3 profiling (DBP), a functional predictive biomarker that measures net changes in mitochondrial apoptotic signaling, to identify anti-apoptotic adaptations upon treatment. We employ this information to guide the use of BH3 mimetics to specifically inhibit BCL-2 pro-survival proteins, defeat resistance and avoid relapse. Indeed, we found that BH3 mimetics that selectively target anti-apoptotic BCL-xL and MCL-1, synergistically enhance the effect of clinically used chemotherapeutic agents vincristine and doxorubicin in RMS cells. We validated this strategy in vivo using a RMS patient-derived xenograft model and observed a reduction in tumor growth with a tendency to stabilization with the sequential combination of vincristine and the MCL-1 inhibitor S63845. We identified the molecular mechanism by which RMS cells acquire resistance to vincristine: an enhanced binding of BID and BAK to MCL-1 after drug exposure, which is suppressed by subsequently adding S63845. Our findings validate the use of DBP as a functional assay to predict treatment effectiveness in RMS and provide a rationale for combining BH3 mimetics with chemotherapeutic agents to avoid tumor resistance, improve treatment efficiency, and decrease undesired secondary effects.

Idioma original	Anglès
Número d’article	634
Pàgines (de-a)	634
Nombre de pàgines	13
Revista	Cell death and disease
Volum	11
Número	8
DOIs	https://doi.org/10.1038/s41419-020-02887-y
Estat de la publicació	Publicada - 1 d’ag. 2020

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10.1038/s41419-020-02887-y

https://ddd.uab.cat/record/252849

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@article{b0299af0fe54467e895b83cb69a9f469,

title = "Sequential combinations of chemotherapeutic agents with BH3 mimetics to treat rhabdomyosarcoma and avoid resistance",

abstract = "Rhabdomyosarcoma (RMS) is the most common soft tissue sarcoma in childhood and adolescence. Refractory/relapsed RMS patients present a bad prognosis that combined with the lack of specific biomarkers impairs the development of new therapies. Here, we utilize dynamic BH3 profiling (DBP), a functional predictive biomarker that measures net changes in mitochondrial apoptotic signaling, to identify anti-apoptotic adaptations upon treatment. We employ this information to guide the use of BH3 mimetics to specifically inhibit BCL-2 pro-survival proteins, defeat resistance and avoid relapse. Indeed, we found that BH3 mimetics that selectively target anti-apoptotic BCL-xL and MCL-1, synergistically enhance the effect of clinically used chemotherapeutic agents vincristine and doxorubicin in RMS cells. We validated this strategy in vivo using a RMS patient-derived xenograft model and observed a reduction in tumor growth with a tendency to stabilization with the sequential combination of vincristine and the MCL-1 inhibitor S63845. We identified the molecular mechanism by which RMS cells acquire resistance to vincristine: an enhanced binding of BID and BAK to MCL-1 after drug exposure, which is suppressed by subsequently adding S63845. Our findings validate the use of DBP as a functional assay to predict treatment effectiveness in RMS and provide a rationale for combining BH3 mimetics with chemotherapeutic agents to avoid tumor resistance, improve treatment efficiency, and decrease undesired secondary effects.",

keywords = "APOPTOSIS, BAK, BCL-2, BCL-X(L), BIOLOGY, CELLS, INDUCTION, INHIBITION, MCL-1, TISSUE",

author = "Clara Alcon and Albert Manzano-Mu{\~n}oz and Estela Prada and Jaume Mora and Aroa Soriano and Gabriela Guill{\'e}n and Soledad Gallego and Josep Roma and Josep Samitier and Alberto Villanueva and Joan Montero",

note = "Funding Information: We would like to thank to Dr. Martinez-Tirado and Dr. Mu{\~n}oz-Pinedo for providing the cell lines used in this study. We would also like to thank the Cytometry Facility from the University of Barcelona for assistance with flow cytometry experiments. This work was supported by the CELLEX foundation and the FERO foundation. The work was partially supported by the Networking Biomedical Research Center (CIBER), Spain. CIBER is an initiative funded by the VI National R\&D\&i Plan 2008–2011, Iniciativa Ingenio 2010, Consolider Program, CIBER Actions, and the Instituto de Salud Carlos III (RD16/0006/0012), with the support of the European Regional Development Fund (ERDF). This work was partially funded by the CERCA Program and by the Commission for Universities and Research of the Department of Innovation, Universities, and Enterprise of the Generalitat de Catalunya (2017 SGR 1079). J.M. acknowledges the Ramon y Cajal Program, Ministerio de Economia y Competitividad (RYC-2015-18357). We also thank http://www.servier.com/Powerpoint-image-bank (licensed under Creative Commons Attribution 3.0 Unported License) for allowing us to use some images to elaborate Fig. 6. Publisher Copyright: {\textcopyright} 2020, The Author(s).Funding Information: We would like to thank to Dr. Martinez-Tirado and Dr. Mu{\~n}oz-Pinedo for providing the cell lines used in this study. We would also like to thank the Cytometry Facility from the University of Barcelona for assistance with flow cytometry experiments. This work was supported by the CELLEX foundation and the FERO foundation. The work was partially supported by the Networking Biomedical Research Center (CIBER), Spain. CIBER is an initiative funded by the VI National R\&D\&i Plan 2008–2011, Iniciativa Ingenio 2010, Consolider Program, CIBER Actions, and the Instituto de Salud Carlos III (RD16/0006/0012), with the support of the European Regional Development Fund (ERDF). This work was partially funded by the CERCA Program and by the Commission for Universities and Research of the Department of Innovation, Universities, and Enterprise of the Generalitat de Catalunya (2017 SGR 1079). J.M. acknowledges the Ramon y Cajal Program, Ministerio de Economia y Competitividad (RYC-2015-18357). We also thank http://www.servier.com/Powerpoint-image-bank (licensed under Creative Commons Attribution 3.0 Unported License) for allowing us to use some images to elaborate Fig. 6. Publisher Copyright: {\textcopyright} 2020, The Author(s).",

year = "2020",

month = aug,

day = "1",

doi = "10.1038/s41419-020-02887-y",

language = "English",

volume = "11",

pages = "634",

journal = "Cell death and disease",

issn = "2041-4889",

publisher = "Springer Nature",

number = "8",

}

TY - JOUR

T1 - Sequential combinations of chemotherapeutic agents with BH3 mimetics to treat rhabdomyosarcoma and avoid resistance

AU - Alcon, Clara

AU - Manzano-Muñoz, Albert

AU - Prada, Estela

AU - Mora, Jaume

AU - Soriano, Aroa

AU - Guillén, Gabriela

AU - Gallego, Soledad

AU - Roma, Josep

AU - Samitier, Josep

AU - Villanueva, Alberto

AU - Montero, Joan

N1 - Funding Information: We would like to thank to Dr. Martinez-Tirado and Dr. Muñoz-Pinedo for providing the cell lines used in this study. We would also like to thank the Cytometry Facility from the University of Barcelona for assistance with flow cytometry experiments. This work was supported by the CELLEX foundation and the FERO foundation. The work was partially supported by the Networking Biomedical Research Center (CIBER), Spain. CIBER is an initiative funded by the VI National R&D&i Plan 2008–2011, Iniciativa Ingenio 2010, Consolider Program, CIBER Actions, and the Instituto de Salud Carlos III (RD16/0006/0012), with the support of the European Regional Development Fund (ERDF). This work was partially funded by the CERCA Program and by the Commission for Universities and Research of the Department of Innovation, Universities, and Enterprise of the Generalitat de Catalunya (2017 SGR 1079). J.M. acknowledges the Ramon y Cajal Program, Ministerio de Economia y Competitividad (RYC-2015-18357). We also thank http://www.servier.com/Powerpoint-image-bank (licensed under Creative Commons Attribution 3.0 Unported License) for allowing us to use some images to elaborate Fig. 6. Publisher Copyright: © 2020, The Author(s).Funding Information: We would like to thank to Dr. Martinez-Tirado and Dr. Muñoz-Pinedo for providing the cell lines used in this study. We would also like to thank the Cytometry Facility from the University of Barcelona for assistance with flow cytometry experiments. This work was supported by the CELLEX foundation and the FERO foundation. The work was partially supported by the Networking Biomedical Research Center (CIBER), Spain. CIBER is an initiative funded by the VI National R&D&i Plan 2008–2011, Iniciativa Ingenio 2010, Consolider Program, CIBER Actions, and the Instituto de Salud Carlos III (RD16/0006/0012), with the support of the European Regional Development Fund (ERDF). This work was partially funded by the CERCA Program and by the Commission for Universities and Research of the Department of Innovation, Universities, and Enterprise of the Generalitat de Catalunya (2017 SGR 1079). J.M. acknowledges the Ramon y Cajal Program, Ministerio de Economia y Competitividad (RYC-2015-18357). We also thank http://www.servier.com/Powerpoint-image-bank (licensed under Creative Commons Attribution 3.0 Unported License) for allowing us to use some images to elaborate Fig. 6. Publisher Copyright: © 2020, The Author(s).

PY - 2020/8/1

Y1 - 2020/8/1

N2 - Rhabdomyosarcoma (RMS) is the most common soft tissue sarcoma in childhood and adolescence. Refractory/relapsed RMS patients present a bad prognosis that combined with the lack of specific biomarkers impairs the development of new therapies. Here, we utilize dynamic BH3 profiling (DBP), a functional predictive biomarker that measures net changes in mitochondrial apoptotic signaling, to identify anti-apoptotic adaptations upon treatment. We employ this information to guide the use of BH3 mimetics to specifically inhibit BCL-2 pro-survival proteins, defeat resistance and avoid relapse. Indeed, we found that BH3 mimetics that selectively target anti-apoptotic BCL-xL and MCL-1, synergistically enhance the effect of clinically used chemotherapeutic agents vincristine and doxorubicin in RMS cells. We validated this strategy in vivo using a RMS patient-derived xenograft model and observed a reduction in tumor growth with a tendency to stabilization with the sequential combination of vincristine and the MCL-1 inhibitor S63845. We identified the molecular mechanism by which RMS cells acquire resistance to vincristine: an enhanced binding of BID and BAK to MCL-1 after drug exposure, which is suppressed by subsequently adding S63845. Our findings validate the use of DBP as a functional assay to predict treatment effectiveness in RMS and provide a rationale for combining BH3 mimetics with chemotherapeutic agents to avoid tumor resistance, improve treatment efficiency, and decrease undesired secondary effects.

AB - Rhabdomyosarcoma (RMS) is the most common soft tissue sarcoma in childhood and adolescence. Refractory/relapsed RMS patients present a bad prognosis that combined with the lack of specific biomarkers impairs the development of new therapies. Here, we utilize dynamic BH3 profiling (DBP), a functional predictive biomarker that measures net changes in mitochondrial apoptotic signaling, to identify anti-apoptotic adaptations upon treatment. We employ this information to guide the use of BH3 mimetics to specifically inhibit BCL-2 pro-survival proteins, defeat resistance and avoid relapse. Indeed, we found that BH3 mimetics that selectively target anti-apoptotic BCL-xL and MCL-1, synergistically enhance the effect of clinically used chemotherapeutic agents vincristine and doxorubicin in RMS cells. We validated this strategy in vivo using a RMS patient-derived xenograft model and observed a reduction in tumor growth with a tendency to stabilization with the sequential combination of vincristine and the MCL-1 inhibitor S63845. We identified the molecular mechanism by which RMS cells acquire resistance to vincristine: an enhanced binding of BID and BAK to MCL-1 after drug exposure, which is suppressed by subsequently adding S63845. Our findings validate the use of DBP as a functional assay to predict treatment effectiveness in RMS and provide a rationale for combining BH3 mimetics with chemotherapeutic agents to avoid tumor resistance, improve treatment efficiency, and decrease undesired secondary effects.

KW - APOPTOSIS

KW - BAK

KW - BCL-2

KW - BCL-X(L)

KW - BIOLOGY

KW - CELLS

KW - INDUCTION

KW - INHIBITION

KW - MCL-1

KW - TISSUE

UR - https://www.scopus.com/pages/publications/85089422639

UR - https://www.mendeley.com/catalogue/cdda7319-d46d-3acb-bdc4-4321d606f0e2/

U2 - 10.1038/s41419-020-02887-y

DO - 10.1038/s41419-020-02887-y

M3 - Article

C2 - 32801295

SN - 2041-4889

VL - 11

SP - 634

JO - Cell death and disease

JF - Cell death and disease

IS - 8

M1 - 634

ER -

Sequential combinations of chemotherapeutic agents with BH3 mimetics to treat rhabdomyosarcoma and avoid resistance

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