A tumor DNA complex aberration index is an independent predictor of survival in breast and ovarian cancer

Hans Kristian Moen Vollan; Oscar M. Rueda; Suet-Feung Chin; Christina Curtis; Gulisa Turashvili; Sohrab P Shah; Ole Christian Lingjaerde; Yinyin Yuan; Charlotte K Ng; Mark J Dunning; Ed Dicks; Elena Provenzano; Stephen Sammut; Steven McKinney; Ian O Ellis; Sarah Pinder; Arnie Purushotham; Leigh C. Murphy; Vessela N. Kristensen; METABRIC Group; James D Brenton; Paul D.P. Pharoah; Anne-Lise Borresen-Dale; Samuel Aparicio; Carlos Caldas

doi:10.1016/j.molonc.2014.07.019

A tumor DNA complex aberration index is an independent predictor of survival in breast and ovarian cancer

Hans Kristian Moen Vollan, Oscar M. Rueda, Suet-Feung Chin, Christina Curtis, Gulisa Turashvili, Sohrab P Shah, Ole Christian Lingjaerde, Yinyin Yuan, Charlotte K Ng, Mark J Dunning, Ed Dicks, Elena Provenzano, Stephen Sammut, Steven McKinney, Ian O Ellis, Sarah Pinder, Arnie Purushotham, Leigh C. Murphy, Vessela N. Kristensen, METABRIC GroupJames D Brenton, Paul D.P. Pharoah, Anne-Lise Borresen-Dale, Samuel Aparicio, Carlos Caldas

Research output: Contribution to journal › Article › Research › peer-review

32 Citations (Scopus)

Abstract

Complex focal chromosomal rearrangements in cancer genomes, also called “firestorms”, can be scored from DNA copy number data. The complex arm‐wise aberration index (CAAI) is a score that captures DNA copy number alterations that appear as focal complex events in tumors, and has potential prognostic value in breast cancer. This study aimed to validate this DNA‐based prognostic index in breast cancer and test for the first time its potential prognostic value in ovarian cancer. Copy number alteration (CNA) data from 1950 breast carcinomas (METABRIC cohort) and 508 high‐grade serous ovarian carcinomas (TCGA dataset) were analyzed. Cases were classified as CAAI positive if at least one complex focal event was scored. Complex alterations were frequently localized on chromosome 8p (n = 159), 17q (n = 176) and 11q (n = 251). CAAI events on 11q were most frequent in estrogen receptor positive (ER+) cases and on 17q in estrogen receptor negative (ER−) cases. We found only a modest correlation between CAAI and the overall rate of genomic instability (GII) and number of breakpoints (r = 0.27 and r = 0.42, p < 0.001). Breast cancer specific survival (BCSS), overall survival (OS) and ovarian cancer progression free survival (PFS) were used as clinical end points in Cox proportional hazard model survival analyses. CAAI positive breast cancers (43%) had higher mortality: hazard ratio (HR) of 1.94 (95%CI, 1.62–2.32) for BCSS, and of 1.49 (95%CI, 1.30–1.71) for OS. Representations of the 70‐gene and the 21‐gene predictors were compared with CAAI in multivariable models and CAAI was independently significant with a Cox adjusted HR of 1.56 (95%CI, 1.23–1.99) for ER+ and 1.55 (95%CI, 1.11–2.18) for ER− disease. None of the expression‐based predictors were prognostic in the ER− subset. We found that a model including CAAI and the two expression‐based prognostic signatures outperformed a model including the 21‐gene and 70‐gene signatures but excluding CAAI. Inclusion of CAAI in the clinical prognostication tool PREDICT significantly improved its performance. CAAI positive ovarian cancers (52%) also had worse prognosis: HRs of 1.3 (95%CI, 1.1–1.7) for PFS and 1.3 (95%CI, 1.1–1.6) for OS. This study validates CAAI as an independent predictor of survival in both ER+ and ER− breast cancer and reveals a significant prognostic value for CAAI in high‐grade serous ovarian cancer.

Original language	English
Pages (from-to)	115-127
Number of pages	13
Journal	Molecular Oncology
Volume	9
Issue number	1
DOIs	https://doi.org/10.1016/j.molonc.2014.07.019
Publication status	Published - 2015
Externally published	Yes

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

Keywords

Breast cancer
Ovarian cancer
Prognostic markers
Biomarker
Genomics
Genomic instability
DNA copy number

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Vollan, H. K. M., Rueda, O. M., Chin, S.-F., Curtis, C., Turashvili, G., Shah, S. P., Lingjaerde, O. C., Yuan, Y., Ng, C. K., Dunning, M. J., Dicks, E., Provenzano, E., Sammut, S., McKinney, S., Ellis, I. O., Pinder, S., Purushotham, A., Murphy, L. C., Kristensen, V. N., ... Caldas, C. (2015). A tumor DNA complex aberration index is an independent predictor of survival in breast and ovarian cancer. Molecular Oncology, 9(1), 115-127. https://doi.org/10.1016/j.molonc.2014.07.019

@article{216b03a8396c4e119ff1009b2cf9acbd,

title = "A tumor DNA complex aberration index is an independent predictor of survival in breast and ovarian cancer",

abstract = "Complex focal chromosomal rearrangements in cancer genomes, also called “firestorms”, can be scored from DNA copy number data. The complex arm‐wise aberration index (CAAI) is a score that captures DNA copy number alterations that appear as focal complex events in tumors, and has potential prognostic value in breast cancer. This study aimed to validate this DNA‐based prognostic index in breast cancer and test for the first time its potential prognostic value in ovarian cancer. Copy number alteration (CNA) data from 1950 breast carcinomas (METABRIC cohort) and 508 high‐grade serous ovarian carcinomas (TCGA dataset) were analyzed. Cases were classified as CAAI positive if at least one complex focal event was scored. Complex alterations were frequently localized on chromosome 8p (n = 159), 17q (n = 176) and 11q (n = 251). CAAI events on 11q were most frequent in estrogen receptor positive (ER+) cases and on 17q in estrogen receptor negative (ER−) cases. We found only a modest correlation between CAAI and the overall rate of genomic instability (GII) and number of breakpoints (r = 0.27 and r = 0.42, p < 0.001). Breast cancer specific survival (BCSS), overall survival (OS) and ovarian cancer progression free survival (PFS) were used as clinical end points in Cox proportional hazard model survival analyses. CAAI positive breast cancers (43\%) had higher mortality: hazard ratio (HR) of 1.94 (95\%CI, 1.62–2.32) for BCSS, and of 1.49 (95\%CI, 1.30–1.71) for OS. Representations of the 70‐gene and the 21‐gene predictors were compared with CAAI in multivariable models and CAAI was independently significant with a Cox adjusted HR of 1.56 (95\%CI, 1.23–1.99) for ER+ and 1.55 (95\%CI, 1.11–2.18) for ER− disease. None of the expression‐based predictors were prognostic in the ER− subset. We found that a model including CAAI and the two expression‐based prognostic signatures outperformed a model including the 21‐gene and 70‐gene signatures but excluding CAAI. Inclusion of CAAI in the clinical prognostication tool PREDICT significantly improved its performance. CAAI positive ovarian cancers (52\%) also had worse prognosis: HRs of 1.3 (95\%CI, 1.1–1.7) for PFS and 1.3 (95\%CI, 1.1–1.6) for OS. This study validates CAAI as an independent predictor of survival in both ER+ and ER− breast cancer and reveals a significant prognostic value for CAAI in high‐grade serous ovarian cancer.",

keywords = "Breast cancer, Ovarian cancer, Prognostic markers, Biomarker, Genomics, Genomic instability, DNA copy number",

author = "Vollan, \{Hans Kristian Moen\} and Rueda, \{Oscar M.\} and Suet-Feung Chin and Christina Curtis and Gulisa Turashvili and Shah, \{Sohrab P\} and Lingjaerde, \{Ole Christian\} and Yinyin Yuan and Ng, \{Charlotte K\} and Dunning, \{Mark J\} and Ed Dicks and Elena Provenzano and Stephen Sammut and Steven McKinney and Ellis, \{Ian O\} and Sarah Pinder and Arnie Purushotham and Murphy, \{Leigh C.\} and Kristensen, \{Vessela N.\} and \{METABRIC Group\} and David Huntsman and Helen Bardwell and Zhihao Ding and Stefan Graf and Linda Jones and Bin Liu and Lynch, \{Andy G\} and Irene Papatheodorou and Gordon Wishart and Steven Chai and Karen Gelmon and Caroline Speers and Peter Watson and Roger Blamey and Green, \{Andrew R\} and Douglas Macmillan and Emad Rakha and Cheryl Gillet and Anita Grigoriadis and \{di Rinaldis\}, Emanuele and Andy Tutt and Michelle Parisien and Sandra Troup and Derek Chan and Claire Fielding and Ana-Teresa Maia and Sarah McGuire and Michelle Osborne and Sara Sayalero and Inmaculada Spiteri and James Hadfield and Lynda Bell and Katie Chow and Nadia Gale and Maria Kovalik and Ying Ng and Prentice, \{Leah M\} and Simon Tavare and Roslin Russell and Samarajiwa, \{Shamith A\} and Doug Speed and Florian Markowetz and Ali Bashashati and Gavin Ha and Gholamreza Haffari and Brenton, \{James D\} and Pharoah, \{Paul D.P.\} and Anne-Lise Borresen-Dale and Samuel Aparicio and Carlos Caldas",

year = "2015",

doi = "10.1016/j.molonc.2014.07.019",

language = "English",

volume = "9",

pages = "115--127",

journal = "Molecular Oncology",

issn = "1574-7891",

publisher = "John Wiley \& Sons",

number = "1",

}

Vollan, HKM, Rueda, OM, Chin, S-F, Curtis, C, Turashvili, G, Shah, SP, Lingjaerde, OC, Yuan, Y, Ng, CK, Dunning, MJ, Dicks, E, Provenzano, E, Sammut, S, McKinney, S, Ellis, IO, Pinder, S, Purushotham, A, Murphy, LC, Kristensen, VN, METABRIC Group, Brenton, JD, Pharoah, PDP, Borresen-Dale, A-L, Aparicio, S & Caldas, C 2015, 'A tumor DNA complex aberration index is an independent predictor of survival in breast and ovarian cancer', Molecular Oncology, vol. 9, no. 1, pp. 115-127. https://doi.org/10.1016/j.molonc.2014.07.019

TY - JOUR

T1 - A tumor DNA complex aberration index is an independent predictor of survival in breast and ovarian cancer

AU - Vollan, Hans Kristian Moen

AU - Rueda, Oscar M.

AU - Chin, Suet-Feung

AU - Curtis, Christina

AU - Turashvili, Gulisa

AU - Shah, Sohrab P

AU - Lingjaerde, Ole Christian

AU - Yuan, Yinyin

AU - Ng, Charlotte K

AU - Dunning, Mark J

AU - Dicks, Ed

AU - Provenzano, Elena

AU - Sammut, Stephen

AU - McKinney, Steven

AU - Ellis, Ian O

AU - Pinder, Sarah

AU - Purushotham, Arnie

AU - Murphy, Leigh C.

AU - Kristensen, Vessela N.

AU - METABRIC Group

AU - Huntsman, David

AU - Bardwell, Helen

AU - Ding, Zhihao

AU - Graf, Stefan

AU - Jones, Linda

AU - Liu, Bin

AU - Lynch, Andy G

AU - Papatheodorou, Irene

AU - Wishart, Gordon

AU - Chai, Steven

AU - Gelmon, Karen

AU - Speers, Caroline

AU - Watson, Peter

AU - Blamey, Roger

AU - Green, Andrew R

AU - Macmillan, Douglas

AU - Rakha, Emad

AU - Gillet, Cheryl

AU - Grigoriadis, Anita

AU - di Rinaldis, Emanuele

AU - Tutt, Andy

AU - Parisien, Michelle

AU - Troup, Sandra

AU - Chan, Derek

AU - Fielding, Claire

AU - Maia, Ana-Teresa

AU - McGuire, Sarah

AU - Osborne, Michelle

AU - Sayalero, Sara

AU - Spiteri, Inmaculada

AU - Hadfield, James

AU - Bell, Lynda

AU - Chow, Katie

AU - Gale, Nadia

AU - Kovalik, Maria

AU - Ng, Ying

AU - Prentice, Leah M

AU - Tavare, Simon

AU - Russell, Roslin

AU - Samarajiwa, Shamith A

AU - Speed, Doug

AU - Markowetz, Florian

AU - Bashashati, Ali

AU - Ha, Gavin

AU - Haffari, Gholamreza

AU - Brenton, James D

AU - Pharoah, Paul D.P.

AU - Borresen-Dale, Anne-Lise

AU - Aparicio, Samuel

AU - Caldas, Carlos

PY - 2015

Y1 - 2015

N2 - Complex focal chromosomal rearrangements in cancer genomes, also called “firestorms”, can be scored from DNA copy number data. The complex arm‐wise aberration index (CAAI) is a score that captures DNA copy number alterations that appear as focal complex events in tumors, and has potential prognostic value in breast cancer. This study aimed to validate this DNA‐based prognostic index in breast cancer and test for the first time its potential prognostic value in ovarian cancer. Copy number alteration (CNA) data from 1950 breast carcinomas (METABRIC cohort) and 508 high‐grade serous ovarian carcinomas (TCGA dataset) were analyzed. Cases were classified as CAAI positive if at least one complex focal event was scored. Complex alterations were frequently localized on chromosome 8p (n = 159), 17q (n = 176) and 11q (n = 251). CAAI events on 11q were most frequent in estrogen receptor positive (ER+) cases and on 17q in estrogen receptor negative (ER−) cases. We found only a modest correlation between CAAI and the overall rate of genomic instability (GII) and number of breakpoints (r = 0.27 and r = 0.42, p < 0.001). Breast cancer specific survival (BCSS), overall survival (OS) and ovarian cancer progression free survival (PFS) were used as clinical end points in Cox proportional hazard model survival analyses. CAAI positive breast cancers (43%) had higher mortality: hazard ratio (HR) of 1.94 (95%CI, 1.62–2.32) for BCSS, and of 1.49 (95%CI, 1.30–1.71) for OS. Representations of the 70‐gene and the 21‐gene predictors were compared with CAAI in multivariable models and CAAI was independently significant with a Cox adjusted HR of 1.56 (95%CI, 1.23–1.99) for ER+ and 1.55 (95%CI, 1.11–2.18) for ER− disease. None of the expression‐based predictors were prognostic in the ER− subset. We found that a model including CAAI and the two expression‐based prognostic signatures outperformed a model including the 21‐gene and 70‐gene signatures but excluding CAAI. Inclusion of CAAI in the clinical prognostication tool PREDICT significantly improved its performance. CAAI positive ovarian cancers (52%) also had worse prognosis: HRs of 1.3 (95%CI, 1.1–1.7) for PFS and 1.3 (95%CI, 1.1–1.6) for OS. This study validates CAAI as an independent predictor of survival in both ER+ and ER− breast cancer and reveals a significant prognostic value for CAAI in high‐grade serous ovarian cancer.

AB - Complex focal chromosomal rearrangements in cancer genomes, also called “firestorms”, can be scored from DNA copy number data. The complex arm‐wise aberration index (CAAI) is a score that captures DNA copy number alterations that appear as focal complex events in tumors, and has potential prognostic value in breast cancer. This study aimed to validate this DNA‐based prognostic index in breast cancer and test for the first time its potential prognostic value in ovarian cancer. Copy number alteration (CNA) data from 1950 breast carcinomas (METABRIC cohort) and 508 high‐grade serous ovarian carcinomas (TCGA dataset) were analyzed. Cases were classified as CAAI positive if at least one complex focal event was scored. Complex alterations were frequently localized on chromosome 8p (n = 159), 17q (n = 176) and 11q (n = 251). CAAI events on 11q were most frequent in estrogen receptor positive (ER+) cases and on 17q in estrogen receptor negative (ER−) cases. We found only a modest correlation between CAAI and the overall rate of genomic instability (GII) and number of breakpoints (r = 0.27 and r = 0.42, p < 0.001). Breast cancer specific survival (BCSS), overall survival (OS) and ovarian cancer progression free survival (PFS) were used as clinical end points in Cox proportional hazard model survival analyses. CAAI positive breast cancers (43%) had higher mortality: hazard ratio (HR) of 1.94 (95%CI, 1.62–2.32) for BCSS, and of 1.49 (95%CI, 1.30–1.71) for OS. Representations of the 70‐gene and the 21‐gene predictors were compared with CAAI in multivariable models and CAAI was independently significant with a Cox adjusted HR of 1.56 (95%CI, 1.23–1.99) for ER+ and 1.55 (95%CI, 1.11–2.18) for ER− disease. None of the expression‐based predictors were prognostic in the ER− subset. We found that a model including CAAI and the two expression‐based prognostic signatures outperformed a model including the 21‐gene and 70‐gene signatures but excluding CAAI. Inclusion of CAAI in the clinical prognostication tool PREDICT significantly improved its performance. CAAI positive ovarian cancers (52%) also had worse prognosis: HRs of 1.3 (95%CI, 1.1–1.7) for PFS and 1.3 (95%CI, 1.1–1.6) for OS. This study validates CAAI as an independent predictor of survival in both ER+ and ER− breast cancer and reveals a significant prognostic value for CAAI in high‐grade serous ovarian cancer.

KW - Breast cancer

KW - Ovarian cancer

KW - Prognostic markers

KW - Biomarker

KW - Genomics

KW - Genomic instability

KW - DNA copy number

UR - https://www.scopus.com/pages/publications/84920448088

U2 - 10.1016/j.molonc.2014.07.019

DO - 10.1016/j.molonc.2014.07.019

M3 - Article

SN - 1574-7891

VL - 9

SP - 115

EP - 127

JO - Molecular Oncology

JF - Molecular Oncology

IS - 1

ER -

A tumor DNA complex aberration index is an independent predictor of survival in breast and ovarian cancer

Abstract

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Keywords

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