FoxM1 insufficiency hyperactivates Ect2–RhoA–mDia1 signaling to drive cancer

Jazeel F. Limzerwala; Karthik B. Jeganathan; Jake A. Kloeber; Brian A. Davies; Cheng Zhang; Ines Sturmlechner; Jian Zhong; Raul Fierro Velasco; Alan P. Fields; Yaxia Yuan; Darren J. Baker; Daohong Zhou; Hu Li; David J. Katzmann; Jan M. van Deursen

doi:10.1038/s43018-020-00116-1

FoxM1 insufficiency hyperactivates Ect2–RhoA–mDia1 signaling to drive cancer

Jazeel F. Limzerwala, Karthik B. Jeganathan, Jake A. Kloeber, Brian A. Davies, Cheng Zhang, Ines Sturmlechner, Jian Zhong, Raul Fierro Velasco, Alan P. Fields, Yaxia Yuan, Darren J. Baker, Daohong Zhou, Hu Li, David J. Katzmann, Jan M. van Deursen

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Resumen

FoxM1 activates genes that regulate S–G2–M cell-cycle progression and, when overexpressed, is associated with poor clinical outcome in multiple cancers. Here we identify FoxM1 as a tumor suppressor in mice that, through its N-terminal domain, binds to and inhibits Ect2 to limit the activity of RhoA GTPase and its effector mDia1, a catalyst of cortical actin nucleation. FoxM1 insufficiency impedes centrosome movement through excessive cortical actin polymerization, thereby causing the formation of nonperpendicular mitotic spindles that missegregate chromosomes and drive tumorigenesis in mice. Importantly, low FOXM1 expression correlates with RhoA GTPase hyperactivity in multiple human cancer types, indicating that suppression of the newly discovered Ect2–RhoA–mDia1 oncogenic axis by FoxM1 is clinically relevant. Furthermore, by dissecting the domain requirements through which FoxM1 inhibits Ect2 guanine nucleotide-exchange factor activity, we provide mechanistic insight for the development of pharmacological approaches that target protumorigenic RhoA activity.

Idioma original	English (US)
Páginas (desde-hasta)	1010-1024
Número de páginas	15
Publicación	Nature Cancer
Volumen	1
N.º	10
DOI	https://doi.org/10.1038/s43018-020-00116-1
Estado	Published - oct 1 2020
Publicado de forma externa	Sí

ASJC Scopus subject areas

Oncology
Cancer Research

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10.1038/s43018-020-00116-1

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Limzerwala, J. F., Jeganathan, K. B., Kloeber, J. A., Davies, B. A., Zhang, C., Sturmlechner, I., Zhong, J., Fierro Velasco, R., Fields, A. P., Yuan, Y., Baker, D. J., Zhou, D., Li, H., Katzmann, D. J., & van Deursen, J. M. (2020). FoxM1 insufficiency hyperactivates Ect2–RhoA–mDia1 signaling to drive cancer. Nature Cancer, 1(10), 1010-1024. https://doi.org/10.1038/s43018-020-00116-1

Limzerwala, JF, Jeganathan, KB, Kloeber, JA, Davies, BA, Zhang, C, Sturmlechner, I, Zhong, J, Fierro Velasco, R, Fields, AP, Yuan, Y, Baker, DJ, Zhou, D, Li, H, Katzmann, DJ & van Deursen, JM 2020, 'FoxM1 insufficiency hyperactivates Ect2–RhoA–mDia1 signaling to drive cancer', Nature Cancer, vol. 1, n.º 10, pp. 1010-1024. https://doi.org/10.1038/s43018-020-00116-1

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title = "FoxM1 insufficiency hyperactivates Ect2–RhoA–mDia1 signaling to drive cancer",

abstract = "FoxM1 activates genes that regulate S–G2–M cell-cycle progression and, when overexpressed, is associated with poor clinical outcome in multiple cancers. Here we identify FoxM1 as a tumor suppressor in mice that, through its N-terminal domain, binds to and inhibits Ect2 to limit the activity of RhoA GTPase and its effector mDia1, a catalyst of cortical actin nucleation. FoxM1 insufficiency impedes centrosome movement through excessive cortical actin polymerization, thereby causing the formation of nonperpendicular mitotic spindles that missegregate chromosomes and drive tumorigenesis in mice. Importantly, low FOXM1 expression correlates with RhoA GTPase hyperactivity in multiple human cancer types, indicating that suppression of the newly discovered Ect2–RhoA–mDia1 oncogenic axis by FoxM1 is clinically relevant. Furthermore, by dissecting the domain requirements through which FoxM1 inhibits Ect2 guanine nucleotide-exchange factor activity, we provide mechanistic insight for the development of pharmacological approaches that target protumorigenic RhoA activity.",

author = "Limzerwala, {Jazeel F.} and Jeganathan, {Karthik B.} and Kloeber, {Jake A.} and Davies, {Brian A.} and Cheng Zhang and Ines Sturmlechner and Jian Zhong and {Fierro Velasco}, Raul and Fields, {Alan P.} and Yaxia Yuan and Baker, {Darren J.} and Daohong Zhou and Hu Li and Katzmann, {David J.} and {van Deursen}, {Jan M.}",

note = "Funding Information: We thank B. Childs, R. Naylor and C. Sieben for helpful discussions, and G. Nelson for managing the mouse colony. We thank the transgenic and gene knockout core at Mayo Clinic for generation of all mutant mouse strains, D. Billadeau (Mayo Clinic, Rochester) for the Cofilin 1 antibody, G. Razidlo (Mayo Clinic, Rochester) for Cytochalasin D and GST-PBD construct, S. Kaufmann (Mayo Clinic, Rochester) for H1299 and A549 cell lines and R. Thaler for assistance with the in vitro GEF activity assay. The human tumor results shown here are in whole or part based upon data generated by TCGA Research Network: https://www.cancer.gov/tcga. This work was supported by NIH grant nos. R01 CA096985, CA126828 and CA168709 to J.M.v.D. J.F.L is supported by Mayo Clinic Graduate School of Biomedical Sciences and J.A.K. by NIH grant no. T32 GM65841. Publisher Copyright: {\textcopyright} 2020, The Author(s), under exclusive licence to Springer Nature America, Inc.",

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AU - Limzerwala, Jazeel F.

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AU - Davies, Brian A.

AU - Zhang, Cheng

AU - Sturmlechner, Ines

AU - Zhong, Jian

AU - Fierro Velasco, Raul

AU - Fields, Alan P.

AU - Yuan, Yaxia

AU - Baker, Darren J.

AU - Zhou, Daohong

AU - Li, Hu

AU - Katzmann, David J.

AU - van Deursen, Jan M.

N1 - Funding Information: We thank B. Childs, R. Naylor and C. Sieben for helpful discussions, and G. Nelson for managing the mouse colony. We thank the transgenic and gene knockout core at Mayo Clinic for generation of all mutant mouse strains, D. Billadeau (Mayo Clinic, Rochester) for the Cofilin 1 antibody, G. Razidlo (Mayo Clinic, Rochester) for Cytochalasin D and GST-PBD construct, S. Kaufmann (Mayo Clinic, Rochester) for H1299 and A549 cell lines and R. Thaler for assistance with the in vitro GEF activity assay. The human tumor results shown here are in whole or part based upon data generated by TCGA Research Network: https://www.cancer.gov/tcga. This work was supported by NIH grant nos. R01 CA096985, CA126828 and CA168709 to J.M.v.D. J.F.L is supported by Mayo Clinic Graduate School of Biomedical Sciences and J.A.K. by NIH grant no. T32 GM65841. Publisher Copyright: © 2020, The Author(s), under exclusive licence to Springer Nature America, Inc.

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N2 - FoxM1 activates genes that regulate S–G2–M cell-cycle progression and, when overexpressed, is associated with poor clinical outcome in multiple cancers. Here we identify FoxM1 as a tumor suppressor in mice that, through its N-terminal domain, binds to and inhibits Ect2 to limit the activity of RhoA GTPase and its effector mDia1, a catalyst of cortical actin nucleation. FoxM1 insufficiency impedes centrosome movement through excessive cortical actin polymerization, thereby causing the formation of nonperpendicular mitotic spindles that missegregate chromosomes and drive tumorigenesis in mice. Importantly, low FOXM1 expression correlates with RhoA GTPase hyperactivity in multiple human cancer types, indicating that suppression of the newly discovered Ect2–RhoA–mDia1 oncogenic axis by FoxM1 is clinically relevant. Furthermore, by dissecting the domain requirements through which FoxM1 inhibits Ect2 guanine nucleotide-exchange factor activity, we provide mechanistic insight for the development of pharmacological approaches that target protumorigenic RhoA activity.

AB - FoxM1 activates genes that regulate S–G2–M cell-cycle progression and, when overexpressed, is associated with poor clinical outcome in multiple cancers. Here we identify FoxM1 as a tumor suppressor in mice that, through its N-terminal domain, binds to and inhibits Ect2 to limit the activity of RhoA GTPase and its effector mDia1, a catalyst of cortical actin nucleation. FoxM1 insufficiency impedes centrosome movement through excessive cortical actin polymerization, thereby causing the formation of nonperpendicular mitotic spindles that missegregate chromosomes and drive tumorigenesis in mice. Importantly, low FOXM1 expression correlates with RhoA GTPase hyperactivity in multiple human cancer types, indicating that suppression of the newly discovered Ect2–RhoA–mDia1 oncogenic axis by FoxM1 is clinically relevant. Furthermore, by dissecting the domain requirements through which FoxM1 inhibits Ect2 guanine nucleotide-exchange factor activity, we provide mechanistic insight for the development of pharmacological approaches that target protumorigenic RhoA activity.

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FoxM1 insufficiency hyperactivates Ect2–RhoA–mDia1 signaling to drive cancer

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