CIP2A Interacts with TopBP1 and Drives Basal-Like Breast Cancer Tumorigenesis

Basal-like breast cancers (BLBC) are characterized by defects in homologous recombination (HR), deficient mitotic checkpoint, and high-proliferation activity. Here, we discover CIP2A as a candidate driver of BLBC. CIP2A was essential for DNA damage–induced initiation of mouse BLBC-like mammary tumor...

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Autores principales: Laine, Anni, Nagelli, Srikar G., Farrington, Caroline, Butt, Umar, Cvrljevic, Anna N., Vainonen, Julia P., Feringa, Femke M., Grönroos, Tove J., Gautam, Prson, Khan, Sofia, Sihto, Harri, Qiao, Xi, Pavic, Karolina, Connolly, Denise C., Kronqvist, Pauliina, Elo, Laura L., Maurer, Jochen, Wennerberg, Krister, Medema, Rene H., Joensuu, Heikki, Peuhu, Emilia, de Visser, Karin, Narla, Goutham, Westermarck, Jukka
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Association for Cancer Research 2021
Materias:
Tumor Biology and Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8373817/
https://www.ncbi.nlm.nih.gov/pubmed/34145035
http://dx.doi.org/10.1158/0008-5472.CAN-20-3651
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author Laine, Anni
Nagelli, Srikar G.
Farrington, Caroline
Butt, Umar
Cvrljevic, Anna N.
Vainonen, Julia P.
Feringa, Femke M.
Grönroos, Tove J.
Gautam, Prson
Khan, Sofia
Sihto, Harri
Qiao, Xi
Pavic, Karolina
Connolly, Denise C.
Kronqvist, Pauliina
Elo, Laura L.
Maurer, Jochen
Wennerberg, Krister
Medema, Rene H.
Joensuu, Heikki
Peuhu, Emilia
de Visser, Karin
Narla, Goutham
Westermarck, Jukka
author_facet Laine, Anni
Nagelli, Srikar G.
Farrington, Caroline
Butt, Umar
Cvrljevic, Anna N.
Vainonen, Julia P.
Feringa, Femke M.
Grönroos, Tove J.
Gautam, Prson
Khan, Sofia
Sihto, Harri
Qiao, Xi
Pavic, Karolina
Connolly, Denise C.
Kronqvist, Pauliina
Elo, Laura L.
Maurer, Jochen
Wennerberg, Krister
Medema, Rene H.
Joensuu, Heikki
Peuhu, Emilia
de Visser, Karin
Narla, Goutham
Westermarck, Jukka
author_sort Laine, Anni
collection PubMed
description Basal-like breast cancers (BLBC) are characterized by defects in homologous recombination (HR), deficient mitotic checkpoint, and high-proliferation activity. Here, we discover CIP2A as a candidate driver of BLBC. CIP2A was essential for DNA damage–induced initiation of mouse BLBC-like mammary tumors and for survival of HR–defective BLBC cells. CIP2A was dispensable for normal mammary gland development and for unperturbed mitosis, but selectively essential for mitotic progression of DNA damaged cells. A direct interaction between CIP2A and a DNA repair scaffold protein TopBP1 was identified, and CIP2A inhibition resulted in enhanced DNA damage–induced TopBP1 and RAD51 recruitment to chromatin in mammary epithelial cells. In addition to its role in tumor initiation, and survival of BRCA-deficient cells, CIP2A also drove proliferative MYC and E2F1 signaling in basal-like triple-negative breast cancer (BL-TNBC) cells. Clinically, high CIP2A expression was associated with poor patient prognosis in BL-TNBCs but not in other breast cancer subtypes. Small-molecule reactivators of PP2A (SMAP) inhibited CIP2A transcription, phenocopied the CIP2A-deficient DNA damage response (DDR), and inhibited growth of patient-derived BLBC xenograft. In summary, these results demonstrate that CIP2A directly interacts with TopBP1 and coordinates DNA damage–induced mitotic checkpoint and proliferation, thereby driving BLBC initiation and progression. SMAPs could serve as a surrogate therapeutic strategy to inhibit the oncogenic activity of CIP2A in BLBCs. SIGNIFICANCE: These results identify CIP2A as a nongenetic driver and therapeutic target in basal-like breast cancer that regulates DNA damage–induced G(2)–M checkpoint and proliferative signaling.
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spelling pubmed-83738172022-02-15 CIP2A Interacts with TopBP1 and Drives Basal-Like Breast Cancer Tumorigenesis Laine, Anni Nagelli, Srikar G. Farrington, Caroline Butt, Umar Cvrljevic, Anna N. Vainonen, Julia P. Feringa, Femke M. Grönroos, Tove J. Gautam, Prson Khan, Sofia Sihto, Harri Qiao, Xi Pavic, Karolina Connolly, Denise C. Kronqvist, Pauliina Elo, Laura L. Maurer, Jochen Wennerberg, Krister Medema, Rene H. Joensuu, Heikki Peuhu, Emilia de Visser, Karin Narla, Goutham Westermarck, Jukka Cancer Res Tumor Biology and Immunology Basal-like breast cancers (BLBC) are characterized by defects in homologous recombination (HR), deficient mitotic checkpoint, and high-proliferation activity. Here, we discover CIP2A as a candidate driver of BLBC. CIP2A was essential for DNA damage–induced initiation of mouse BLBC-like mammary tumors and for survival of HR–defective BLBC cells. CIP2A was dispensable for normal mammary gland development and for unperturbed mitosis, but selectively essential for mitotic progression of DNA damaged cells. A direct interaction between CIP2A and a DNA repair scaffold protein TopBP1 was identified, and CIP2A inhibition resulted in enhanced DNA damage–induced TopBP1 and RAD51 recruitment to chromatin in mammary epithelial cells. In addition to its role in tumor initiation, and survival of BRCA-deficient cells, CIP2A also drove proliferative MYC and E2F1 signaling in basal-like triple-negative breast cancer (BL-TNBC) cells. Clinically, high CIP2A expression was associated with poor patient prognosis in BL-TNBCs but not in other breast cancer subtypes. Small-molecule reactivators of PP2A (SMAP) inhibited CIP2A transcription, phenocopied the CIP2A-deficient DNA damage response (DDR), and inhibited growth of patient-derived BLBC xenograft. In summary, these results demonstrate that CIP2A directly interacts with TopBP1 and coordinates DNA damage–induced mitotic checkpoint and proliferation, thereby driving BLBC initiation and progression. SMAPs could serve as a surrogate therapeutic strategy to inhibit the oncogenic activity of CIP2A in BLBCs. SIGNIFICANCE: These results identify CIP2A as a nongenetic driver and therapeutic target in basal-like breast cancer that regulates DNA damage–induced G(2)–M checkpoint and proliferative signaling. American Association for Cancer Research 2021-08-15 2021-06-18 /pmc/articles/PMC8373817/ /pubmed/34145035 http://dx.doi.org/10.1158/0008-5472.CAN-20-3651 Text en ©2021 The Authors; Published by the American Association for Cancer Research https://creativecommons.org/licenses/by-nc-nd/4.0/This open access article is distributed under the Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International (CC BY-NC-ND 4.0) license.
spellingShingle Tumor Biology and Immunology
Laine, Anni
Nagelli, Srikar G.
Farrington, Caroline
Butt, Umar
Cvrljevic, Anna N.
Vainonen, Julia P.
Feringa, Femke M.
Grönroos, Tove J.
Gautam, Prson
Khan, Sofia
Sihto, Harri
Qiao, Xi
Pavic, Karolina
Connolly, Denise C.
Kronqvist, Pauliina
Elo, Laura L.
Maurer, Jochen
Wennerberg, Krister
Medema, Rene H.
Joensuu, Heikki
Peuhu, Emilia
de Visser, Karin
Narla, Goutham
Westermarck, Jukka
CIP2A Interacts with TopBP1 and Drives Basal-Like Breast Cancer Tumorigenesis
title CIP2A Interacts with TopBP1 and Drives Basal-Like Breast Cancer Tumorigenesis
title_full CIP2A Interacts with TopBP1 and Drives Basal-Like Breast Cancer Tumorigenesis
title_fullStr CIP2A Interacts with TopBP1 and Drives Basal-Like Breast Cancer Tumorigenesis
title_full_unstemmed CIP2A Interacts with TopBP1 and Drives Basal-Like Breast Cancer Tumorigenesis
title_short CIP2A Interacts with TopBP1 and Drives Basal-Like Breast Cancer Tumorigenesis
title_sort cip2a interacts with topbp1 and drives basal-like breast cancer tumorigenesis
topic Tumor Biology and Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8373817/
https://www.ncbi.nlm.nih.gov/pubmed/34145035
http://dx.doi.org/10.1158/0008-5472.CAN-20-3651
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