Concomitant inactivation of the p53- and pRB- functional pathways predicts resistance to DNA damaging drugs in breast cancer in vivo

Stian Knappskog; Elisabet O Berge; Ranjan Chrisanthar; Stephanie Geisler; Vidar Staalesen; Beryl Leirvaag; Synnøve Yndestad; Elise de Faveri; Bård O Karlsen; David C Wedge; Lars A Akslen; Peer K Lilleng; Erik Løkkevik; Steinar Lundgren; Bjørn Østenstad; Terje Risberg; Ingvild Mjaaland; Turid Aas; Per E Lønning

doi:10.1016/j.molonc.2015.04.008

Concomitant inactivation of the p53- and pRB- functional pathways predicts resistance to DNA damaging drugs in breast cancer in vivo

Mol Oncol. 2015 Oct;9(8):1553-64. doi: 10.1016/j.molonc.2015.04.008. Epub 2015 May 8.

Authors

Stian Knappskog¹, Elisabet O Berge², Ranjan Chrisanthar², Stephanie Geisler², Vidar Staalesen², Beryl Leirvaag², Synnøve Yndestad², Elise de Faveri², Bård O Karlsen³, David C Wedge⁴, Lars A Akslen⁵, Peer K Lilleng⁶, Erik Løkkevik⁷, Steinar Lundgren⁸, Bjørn Østenstad⁹, Terje Risberg¹⁰, Ingvild Mjaaland¹¹, Turid Aas¹², Per E Lønning²

Affiliations

¹ Section of Oncology, Department of Clinical Science, University of Bergen, Norway; Department of Oncology, Haukeland University Hospital, Bergen, Norway. Electronic address: stian.knappskog@k2.uib.no.
² Section of Oncology, Department of Clinical Science, University of Bergen, Norway; Department of Oncology, Haukeland University Hospital, Bergen, Norway.
³ Department of Oncology, Haukeland University Hospital, Bergen, Norway.
⁴ Wellcome Trust Sanger Institute, Hinxton, Cambridgeshire, UK.
⁵ Centre for Cancer Biomarkers (CCBIO), Department of Clinical Medicine, University of Bergen, Norway; Department of Pathology, Haukeland University Hospital, Bergen, Norway.
⁶ Department of Pathology, Haukeland University Hospital, Bergen, Norway; The Gade Laboratory for Pathology, Department of Clinical Medicine, University of Bergen, Norway.
⁷ Department of Oncology, Oslo University Hospital, The Norwegian Radium Hospital, Oslo, Norway.
⁸ Department of Oncology, St. Olavs University Hospital, Trondheim, Norway; Department of Cancer Research and Molecular Medicine, Norwegian University of Science and Technology, Trondheim, Norway.
⁹ Department of Oncology, Oslo University Hospital, Ullevaal, Oslo, Norway.
¹⁰ Department of Oncology, University Hospital of Northern Norway and Institute of Clinical Medicine, University of Tromsø, Tromsø, Norway.
¹¹ Division of Hematology and Oncology, Stavanger University Hospital, Stavanger, Norway.
¹² Department of Surgery, Haukeland University Hospital, Bergen, Norway.

Abstract

Chemoresistance is the main obstacle to cancer cure. Contrasting studies focusing on single gene mutations, we hypothesize chemoresistance to be due to inactivation of key pathways affecting cellular mechanisms such as apoptosis, senescence, or DNA repair. In support of this hypothesis, we have previously shown inactivation of either TP53 or its key activators CHK2 and ATM to predict resistance to DNA damaging drugs in breast cancer better than TP53 mutations alone. Further, we hypothesized that redundant pathway(s) may compensate for loss of p53-pathway signaling and that these are inactivated as well in resistant tumour cells. Here, we assessed genetic alterations of the retinoblastoma gene (RB1) and its key regulators: Cyclin D and E as well as their inhibitors p16 and p27. In an exploratory cohort of 69 patients selected from two prospective studies treated with either doxorubicin monotherapy or 5-FU and mitomycin for locally advanced breast cancers, we found defects in the pRB-pathway to be associated with therapy resistance (p-values ranging from 0.001 to 0.094, depending on the cut-off value applied to p27 expression levels). Although statistically weaker, we observed confirmatory associations in a validation cohort from another prospective study (n = 107 patients treated with neoadjuvant epirubicin monotherapy; p-values ranging from 7.0 × 10(-4) to 0.001 in the combined data sets). Importantly, inactivation of the p53-and the pRB-pathways in concert predicted resistance to therapy more strongly than each of the two pathways assessed individually (exploratory cohort: p-values ranging from 3.9 × 10(-6) to 7.5 × 10(-3) depending on cut-off values applied to ATM and p27 mRNA expression levels). Again, similar findings were confirmed in the validation cohort, with p-values ranging from 6.0 × 10(-7) to 6.5 × 10(-5) in the combined data sets. Our findings strongly indicate that concomitant inactivation of the p53- and pRB- pathways predict resistance towards anthracyclines and mitomycin in breast cancer in vivo.

Keywords: Breast cancer; Resistance; p53; pRB.

Publication types

Research Support, Non-U.S. Gov't
Validation Study

MeSH terms

Antibiotics, Antineoplastic / therapeutic use*
Breast Neoplasms / diagnosis*
Breast Neoplasms / genetics*
Cohort Studies
DNA Damage* / genetics
DNA Mutational Analysis
Doxorubicin / therapeutic use
Drug Resistance, Neoplasm / genetics*
Female
Fluorouracil / therapeutic use
Gene Expression Regulation, Neoplastic
Gene Silencing
Humans
Mitomycin / therapeutic use
Prognosis
Retinoblastoma Protein / genetics*
Retinoblastoma Protein / metabolism
Signal Transduction / genetics
Treatment Failure
Tumor Suppressor Protein p53 / genetics*

Substances

Antibiotics, Antineoplastic
Retinoblastoma Protein
TP53 protein, human
Tumor Suppressor Protein p53
Mitomycin
Doxorubicin
Fluorouracil