Subsequent female breast cancer risk associated with anthracycline chemotherapy for childhood cancer

Yuehan Wang; C. cile M. Ronckers; Flora E. van Leeuwen; Chaya S. Moskowitz; Wendy Leisenring; Gregory T. Armstrong; Florent de Vathaire; Melissa M. Hudson; Claudia E. Kuehni; Michael A. Arnold; Charlotte Demoor-Goldschmidt; Daniel M. Green; Tara O. Henderson; Rebecca M. Howell; Matthew J. Ehrhardt; Joseph P. Neglia; Kevin C. Oeffinger; Helena J. H. van der Pal; Leslie L. Robison; Michael Schaapveld; Lucie M. Turcotte; Nicolas Waespe; Leontien C. M. Kremer; Jop C. Teepen; Flora E. van Leeuwen; Florent de Vathaire; Helena J. H. van der Pal; Nadia Haddy; Ibrahima Diallo; K. Scott Baker; Amy Berrington de González; Miriam R. Conces; Louis S. Constine; Mike Hawkins; Jacqueline J. Loonen; Marloes Louwerens; Geert O. Janssens; Lene Mellemkjaer; Raoul Reulen; Jeanette F. Winther

doi:10.1038/s41591-023-02514-1

Subsequent female breast cancer risk associated with anthracycline chemotherapy for childhood cancer

Yuehan Wang^*
, C. cile M. Ronckers
, Flora E. van Leeuwen
, Chaya S. Moskowitz
, Wendy Leisenring
, Gregory T. Armstrong
, Florent de Vathaire
, Melissa M. Hudson
, Claudia E. Kuehni
, Michael A. Arnold
, Charlotte Demoor-Goldschmidt
, Daniel M. Green
, Tara O. Henderson
, Rebecca M. Howell
, Matthew J. Ehrhardt
, Joseph P. Neglia
, Kevin C. Oeffinger
, Helena J. H. van der Pal
, Leslie L. Robison
, Michael Schaapveld

Lucie M. Turcotte, Nicolas Waespe, Leontien C. M. Kremer, Jop C. Teepen, Flora E. van Leeuwen, Florent de Vathaire, Helena J. H. van der Pal, Nadia Haddy, Ibrahima Diallo, K. Scott Baker, Amy Berrington de González, Miriam R. Conces, Louis S. Constine, Mike Hawkins, Jacqueline J. Loonen, Marloes Louwerens, Geert O. Janssens, Lene Mellemkjaer, Raoul Reulen, Jeanette F. Winther

^*Corresponding author for this work

Princess Máxima Center for Pediatric Oncology
University of Oldenburg
Johannes Gutenberg University Mainz
Netherlands Cancer Institute
Memorial Sloan-Kettering Cancer Center
Fred Hutchinson Cancer Research Center
St. Jude Children Research Hospital
Université Paris-Sud
University of Bern
University Children’s Hospital Bern, Inselspital, University of Bern, Switzerland.
Children's Hospital Colorado
University of Colorado Anschutz Medical Campus
Université d'Angers
Department of Radiotherapy, François Baclesse Center, Caen, France
The University of Chicago
University of Texas MD Anderson Cancer Center
University of Minnesota Twin Cities
Duke University
University of Geneva
Utrecht University
National Institutes of Health
Oncogenetics Team, The Institute of Cancer Research, London, United Kingdom
Institute for Genomic Medicine, Nationwide Children’s Hospital, Columbus, OH, 43205, USA
Ohio State University
University of Rochester
University of Birmingham
Radboud University Medical Center
Leiden University Medical Center
University Medical Center Utrecht
Danish Cancer Society
Aarhus University

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Abstract

Anthracycline-based chemotherapy is associated with increased subsequent breast cancer (SBC) risk in female childhood cancer survivors, but the current evidence is insufficient to support early breast cancer screening recommendations for survivors treated with anthracyclines. In this study, we pooled individual patient data of 17,903 survivors from six well-established studies, of whom 782 (4.4%) developed a SBC, and analyzed dose-dependent effects of individual anthracycline agents on developing SBC and interactions with chest radiotherapy. A dose-dependent increased SBC risk was seen for doxorubicin (hazard ratio (HR) per 100 mg m−2: 1.24, 95% confidence interval (CI): 1.18–1.31), with more than twofold increased risk for survivors treated with ≥200 mg m−2 cumulative doxorubicin dose versus no doxorubicin (HR: 2.50 for 200–299 mg m−2, HR: 2.33 for 300–399 mg m−2 and HR: 2.78 for ≥400 mg m−2). For daunorubicin, the associations were not statistically significant. Epirubicin was associated with increased SBC risk (yes/no, HR: 3.25, 95% CI: 1.59–6.63). For patients treated with or without chest irradiation, HRs per 100 mg m−2 of doxorubicin were 1.11 (95% CI: 1.02–1.21) and 1.26 (95% CI: 1.17–1.36), respectively. Our findings support that early initiation of SBC surveillance may be reasonable for survivors who received ≥200 mg m−2 cumulative doxorubicin dose and should be considered in SBC surveillance guidelines for survivors and future treatment protocols.

Original language	English
Pages (from-to)	2268-2277
Number of pages	10
Journal	Nature medicine
Volume	29
Issue number	9
Early online date	2023
DOIs	https://doi.org/10.1038/s41591-023-02514-1
Publication status	Published - Sept 2023

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Wang, Y., Ronckers, C. C. M., van Leeuwen, F. E., Moskowitz, C. S., Leisenring, W., Armstrong, G. T., de Vathaire, F., Hudson, M. M., Kuehni, C. E., Arnold, M. A., Demoor-Goldschmidt, C., Green, D. M., Henderson, T. O., Howell, R. M., Ehrhardt, M. J., Neglia, J. P., Oeffinger, K. C., van der Pal, H. J. H., Robison, L. L., ... Winther, J. F. (2023). Subsequent female breast cancer risk associated with anthracycline chemotherapy for childhood cancer. Nature medicine, 29(9), 2268-2277. https://doi.org/10.1038/s41591-023-02514-1

@article{8929afd937e2480797549e57b2212395,

title = "Subsequent female breast cancer risk associated with anthracycline chemotherapy for childhood cancer",

abstract = "Anthracycline-based chemotherapy is associated with increased subsequent breast cancer (SBC) risk in female childhood cancer survivors, but the current evidence is insufficient to support early breast cancer screening recommendations for survivors treated with anthracyclines. In this study, we pooled individual patient data of 17,903 survivors from six well-established studies, of whom 782 (4.4\%) developed a SBC, and analyzed dose-dependent effects of individual anthracycline agents on developing SBC and interactions with chest radiotherapy. A dose-dependent increased SBC risk was seen for doxorubicin (hazard ratio (HR) per 100 mg m−2: 1.24, 95\% confidence interval (CI): 1.18–1.31), with more than twofold increased risk for survivors treated with ≥200 mg m−2 cumulative doxorubicin dose versus no doxorubicin (HR: 2.50 for 200–299 mg m−2, HR: 2.33 for 300–399 mg m−2 and HR: 2.78 for ≥400 mg m−2). For daunorubicin, the associations were not statistically significant. Epirubicin was associated with increased SBC risk (yes/no, HR: 3.25, 95\% CI: 1.59–6.63). For patients treated with or without chest irradiation, HRs per 100 mg m−2 of doxorubicin were 1.11 (95\% CI: 1.02–1.21) and 1.26 (95\% CI: 1.17–1.36), respectively. Our findings support that early initiation of SBC surveillance may be reasonable for survivors who received ≥200 mg m−2 cumulative doxorubicin dose and should be considered in SBC surveillance guidelines for survivors and future treatment protocols.",

author = "Yuehan Wang and Ronckers, \{C. cile M.\} and \{van Leeuwen\}, \{Flora E.\} and Moskowitz, \{Chaya S.\} and Wendy Leisenring and Armstrong, \{Gregory T.\} and \{de Vathaire\}, Florent and Hudson, \{Melissa M.\} and Kuehni, \{Claudia E.\} and Arnold, \{Michael A.\} and Charlotte Demoor-Goldschmidt and Green, \{Daniel M.\} and Henderson, \{Tara O.\} and Howell, \{Rebecca M.\} and Ehrhardt, \{Matthew J.\} and Neglia, \{Joseph P.\} and Oeffinger, \{Kevin C.\} and \{van der Pal\}, \{Helena J. H.\} and Robison, \{Leslie L.\} and Michael Schaapveld and Turcotte, \{Lucie M.\} and Nicolas Waespe and Kremer, \{Leontien C. M.\} and Teepen, \{Jop C.\} and \{van Leeuwen\}, \{Flora E.\} and \{de Vathaire\}, Florent and \{van der Pal\}, \{Helena J. H.\} and Nadia Haddy and Ibrahima Diallo and Baker, \{K. Scott\} and \{de Gonz{\'a}lez\}, \{Amy Berrington\} and Conces, \{Miriam R.\} and Constine, \{Louis S.\} and Mike Hawkins and Loonen, \{Jacqueline J.\} and Marloes Louwerens and Janssens, \{Geert O.\} and Lene Mellemkjaer and Raoul Reulen and Winther, \{Jeanette F.\}",

note = "Funding Information: This work was supported by the Children Cancer Free Foundation (KiKa; grant 325 title: risk factors for female breast cancer after treatment for childhood and adolescent cancer: individual patient data analyses of an internationally pooled cohort) to C.M.R., F.E.v.L., L.C.M.K. (principal investigators). The CCSS and SJLIFE cohorts are supported by the National Cancer Institute (CA55727 to G.T.A. (principal investigator) and CA195547 to M.M.H. and K.K.N. (principal investigators)) as well as support to St. Jude Children{\textquoteright}s Research Hospital also provided by the Cancer Center Support (CORE) grant (CA21765 to C.R. (principal investigator)) and the American Lebanese-Syrian Associated Charities (ALSAC). The NWTSG was supported by the National Cancer Institute (CA054498 to N.E.B. and W.L. (principal investigator)). The DCCSS-LATER is supported by the Dutch Cancer Society (DCOG2011-5027 to C.M.R., F.E.v.L. and W.T. (principal investigators) and UVA2012-5517 to C.M.R. and L.C.M.K. (principal investigators)). The FCCSS is funded by the Fondation ARC (PopHARC Grant to F.d.V. (principal investigator)), the Agence Nationale pour la Recherche M{\'e}dicale (ANR, Hope-Epi Grant to F.d.V. (principal investigator)), and the Gustave Roussy Foundation (Pediatric Program {\textquoteleft}Gu{\'e}rir le Cancer de l{\textquoteright}Enfant{\textquoteright} to F.d.V. (principal investigator)). The SCCSS has been supported by the Swiss Cancer League and the Swiss Cancer Research foundation (KFS-02783-02-2011, KLS-3412-02-2014, KFS-4157-02-2017, KLS/KFS-4825-01-2019, KFS-4722-02-2019, KFS-5027-02-2020, KFS-5302-02-2021 and KLS-5432-08-2021 to C.E.K. (principal investigator)), Kinderkrebs Schweiz ( www.kinderkrebs-schweiz.ch ) and Kinderkrebshilfe Schweiz ( www.kinderkrebshilfe.ch ). The Dutch Hodgkin Late Effects cohort has been supported by the Dutch Cancer Society (NKI 2010-4720 to F.E.v.L. (principal investigator)). Publisher Copyright: {\textcopyright} 2023, The Author(s).",

year = "2023",

month = sep,

doi = "10.1038/s41591-023-02514-1",

language = "English",

volume = "29",

pages = "2268--2277",

journal = "Nature medicine",

issn = "1078-8956",

publisher = "Nature Publishing Group",

number = "9",

}

Wang, Y, Ronckers, CCM, van Leeuwen, FE, Moskowitz, CS, Leisenring, W, Armstrong, GT, de Vathaire, F, Hudson, MM, Kuehni, CE, Arnold, MA, Demoor-Goldschmidt, C, Green, DM, Henderson, TO, Howell, RM, Ehrhardt, MJ, Neglia, JP, Oeffinger, KC, van der Pal, HJH, Robison, LL, Schaapveld, M, Turcotte, LM, Waespe, N, Kremer, LCM, Teepen, JC, van Leeuwen, FE, de Vathaire, F, van der Pal, HJH, Haddy, N, Diallo, I, Baker, KS, de González, AB, Conces, MR, Constine, LS, Hawkins, M, Loonen, JJ, Louwerens, M, Janssens, GO, Mellemkjaer, L, Reulen, R & Winther, JF 2023, 'Subsequent female breast cancer risk associated with anthracycline chemotherapy for childhood cancer', Nature medicine, vol. 29, no. 9, pp. 2268-2277. https://doi.org/10.1038/s41591-023-02514-1

TY - JOUR

T1 - Subsequent female breast cancer risk associated with anthracycline chemotherapy for childhood cancer

AU - Wang, Yuehan

AU - Ronckers, C. cile M.

AU - van Leeuwen, Flora E.

AU - Moskowitz, Chaya S.

AU - Leisenring, Wendy

AU - Armstrong, Gregory T.

AU - de Vathaire, Florent

AU - Hudson, Melissa M.

AU - Kuehni, Claudia E.

AU - Arnold, Michael A.

AU - Demoor-Goldschmidt, Charlotte

AU - Green, Daniel M.

AU - Henderson, Tara O.

AU - Howell, Rebecca M.

AU - Ehrhardt, Matthew J.

AU - Neglia, Joseph P.

AU - Oeffinger, Kevin C.

AU - van der Pal, Helena J. H.

AU - Robison, Leslie L.

AU - Schaapveld, Michael

AU - Turcotte, Lucie M.

AU - Waespe, Nicolas

AU - Kremer, Leontien C. M.

AU - Teepen, Jop C.

AU - van Leeuwen, Flora E.

AU - de Vathaire, Florent

AU - van der Pal, Helena J. H.

AU - Haddy, Nadia

AU - Diallo, Ibrahima

AU - Baker, K. Scott

AU - de González, Amy Berrington

AU - Conces, Miriam R.

AU - Constine, Louis S.

AU - Hawkins, Mike

AU - Loonen, Jacqueline J.

AU - Louwerens, Marloes

AU - Janssens, Geert O.

AU - Mellemkjaer, Lene

AU - Reulen, Raoul

AU - Winther, Jeanette F.

N1 - Funding Information: This work was supported by the Children Cancer Free Foundation (KiKa; grant 325 title: risk factors for female breast cancer after treatment for childhood and adolescent cancer: individual patient data analyses of an internationally pooled cohort) to C.M.R., F.E.v.L., L.C.M.K. (principal investigators). The CCSS and SJLIFE cohorts are supported by the National Cancer Institute (CA55727 to G.T.A. (principal investigator) and CA195547 to M.M.H. and K.K.N. (principal investigators)) as well as support to St. Jude Children’s Research Hospital also provided by the Cancer Center Support (CORE) grant (CA21765 to C.R. (principal investigator)) and the American Lebanese-Syrian Associated Charities (ALSAC). The NWTSG was supported by the National Cancer Institute (CA054498 to N.E.B. and W.L. (principal investigator)). The DCCSS-LATER is supported by the Dutch Cancer Society (DCOG2011-5027 to C.M.R., F.E.v.L. and W.T. (principal investigators) and UVA2012-5517 to C.M.R. and L.C.M.K. (principal investigators)). The FCCSS is funded by the Fondation ARC (PopHARC Grant to F.d.V. (principal investigator)), the Agence Nationale pour la Recherche Médicale (ANR, Hope-Epi Grant to F.d.V. (principal investigator)), and the Gustave Roussy Foundation (Pediatric Program ‘Guérir le Cancer de l’Enfant’ to F.d.V. (principal investigator)). The SCCSS has been supported by the Swiss Cancer League and the Swiss Cancer Research foundation (KFS-02783-02-2011, KLS-3412-02-2014, KFS-4157-02-2017, KLS/KFS-4825-01-2019, KFS-4722-02-2019, KFS-5027-02-2020, KFS-5302-02-2021 and KLS-5432-08-2021 to C.E.K. (principal investigator)), Kinderkrebs Schweiz ( www.kinderkrebs-schweiz.ch ) and Kinderkrebshilfe Schweiz ( www.kinderkrebshilfe.ch ). The Dutch Hodgkin Late Effects cohort has been supported by the Dutch Cancer Society (NKI 2010-4720 to F.E.v.L. (principal investigator)). Publisher Copyright: © 2023, The Author(s).

PY - 2023/9

Y1 - 2023/9

N2 - Anthracycline-based chemotherapy is associated with increased subsequent breast cancer (SBC) risk in female childhood cancer survivors, but the current evidence is insufficient to support early breast cancer screening recommendations for survivors treated with anthracyclines. In this study, we pooled individual patient data of 17,903 survivors from six well-established studies, of whom 782 (4.4%) developed a SBC, and analyzed dose-dependent effects of individual anthracycline agents on developing SBC and interactions with chest radiotherapy. A dose-dependent increased SBC risk was seen for doxorubicin (hazard ratio (HR) per 100 mg m−2: 1.24, 95% confidence interval (CI): 1.18–1.31), with more than twofold increased risk for survivors treated with ≥200 mg m−2 cumulative doxorubicin dose versus no doxorubicin (HR: 2.50 for 200–299 mg m−2, HR: 2.33 for 300–399 mg m−2 and HR: 2.78 for ≥400 mg m−2). For daunorubicin, the associations were not statistically significant. Epirubicin was associated with increased SBC risk (yes/no, HR: 3.25, 95% CI: 1.59–6.63). For patients treated with or without chest irradiation, HRs per 100 mg m−2 of doxorubicin were 1.11 (95% CI: 1.02–1.21) and 1.26 (95% CI: 1.17–1.36), respectively. Our findings support that early initiation of SBC surveillance may be reasonable for survivors who received ≥200 mg m−2 cumulative doxorubicin dose and should be considered in SBC surveillance guidelines for survivors and future treatment protocols.

AB - Anthracycline-based chemotherapy is associated with increased subsequent breast cancer (SBC) risk in female childhood cancer survivors, but the current evidence is insufficient to support early breast cancer screening recommendations for survivors treated with anthracyclines. In this study, we pooled individual patient data of 17,903 survivors from six well-established studies, of whom 782 (4.4%) developed a SBC, and analyzed dose-dependent effects of individual anthracycline agents on developing SBC and interactions with chest radiotherapy. A dose-dependent increased SBC risk was seen for doxorubicin (hazard ratio (HR) per 100 mg m−2: 1.24, 95% confidence interval (CI): 1.18–1.31), with more than twofold increased risk for survivors treated with ≥200 mg m−2 cumulative doxorubicin dose versus no doxorubicin (HR: 2.50 for 200–299 mg m−2, HR: 2.33 for 300–399 mg m−2 and HR: 2.78 for ≥400 mg m−2). For daunorubicin, the associations were not statistically significant. Epirubicin was associated with increased SBC risk (yes/no, HR: 3.25, 95% CI: 1.59–6.63). For patients treated with or without chest irradiation, HRs per 100 mg m−2 of doxorubicin were 1.11 (95% CI: 1.02–1.21) and 1.26 (95% CI: 1.17–1.36), respectively. Our findings support that early initiation of SBC surveillance may be reasonable for survivors who received ≥200 mg m−2 cumulative doxorubicin dose and should be considered in SBC surveillance guidelines for survivors and future treatment protocols.

UR - https://www.scopus.com/pages/publications/85170522025

U2 - 10.1038/s41591-023-02514-1

DO - 10.1038/s41591-023-02514-1

M3 - Article

C2 - 37696934

SN - 1078-8956

VL - 29

SP - 2268

EP - 2277

JO - Nature medicine

JF - Nature medicine

IS - 9

ER -

Subsequent female breast cancer risk associated with anthracycline chemotherapy for childhood cancer

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