ERα-associated translocations underlie oncogene amplifications in breast cancer

Focal copy-number amplification is an oncogenic event. Although recent studies have revealed the complex structure(1–3) and the evolutionary trajectories(4) of oncogene amplicons, their origin remains poorly understood. Here we show that focal amplifications in breast cancer frequently derive from a...

Descripción completa

Detalles Bibliográficos
Autores principales: Lee, Jake June-Koo, Jung, Youngsook Lucy, Cheong, Taek-Chin, Espejo Valle-Inclan, Jose, Chu, Chong, Gulhan, Doga C., Ljungström, Viktor, Jin, Hu, Viswanadham, Vinayak V., Watson, Emma V., Cortés-Ciriano, Isidro, Elledge, Stephen J., Chiarle, Roberto, Pellman, David, Park, Peter J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Nature Publishing Group UK 2023
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10307628/
https://www.ncbi.nlm.nih.gov/pubmed/37198482
http://dx.doi.org/10.1038/s41586-023-06057-w
_version_ 1785066074316734464
author Lee, Jake June-Koo
Jung, Youngsook Lucy
Cheong, Taek-Chin
Espejo Valle-Inclan, Jose
Chu, Chong
Gulhan, Doga C.
Ljungström, Viktor
Jin, Hu
Viswanadham, Vinayak V.
Watson, Emma V.
Cortés-Ciriano, Isidro
Elledge, Stephen J.
Chiarle, Roberto
Pellman, David
Park, Peter J.
author_facet Lee, Jake June-Koo
Jung, Youngsook Lucy
Cheong, Taek-Chin
Espejo Valle-Inclan, Jose
Chu, Chong
Gulhan, Doga C.
Ljungström, Viktor
Jin, Hu
Viswanadham, Vinayak V.
Watson, Emma V.
Cortés-Ciriano, Isidro
Elledge, Stephen J.
Chiarle, Roberto
Pellman, David
Park, Peter J.
author_sort Lee, Jake June-Koo
collection PubMed
description Focal copy-number amplification is an oncogenic event. Although recent studies have revealed the complex structure(1–3) and the evolutionary trajectories(4) of oncogene amplicons, their origin remains poorly understood. Here we show that focal amplifications in breast cancer frequently derive from a mechanism—which we term translocation–bridge amplification—involving inter-chromosomal translocations that lead to dicentric chromosome bridge formation and breakage. In 780 breast cancer genomes, we observe that focal amplifications are frequently connected to each other by inter-chromosomal translocations at their boundaries. Subsequent analysis indicates the following model: the oncogene neighbourhood is translocated in G1 creating a dicentric chromosome, the dicentric chromosome is replicated, and as dicentric sister chromosomes segregate during mitosis, a chromosome bridge is formed and then broken, with fragments often being circularized in extrachromosomal DNAs. This model explains the amplifications of key oncogenes, including ERBB2 and CCND1. Recurrent amplification boundaries and rearrangement hotspots correlate with oestrogen receptor binding in breast cancer cells. Experimentally, oestrogen treatment induces DNA double-strand breaks in the oestrogen receptor target regions that are repaired by translocations, suggesting a role of oestrogen in generating the initial translocations. A pan-cancer analysis reveals tissue-specific biases in mechanisms initiating focal amplifications, with the breakage–fusion–bridge cycle prevalent in some and the translocation–bridge amplification in others, probably owing to the different timing of DNA break repair. Our results identify a common mode of oncogene amplification and propose oestrogen as its mechanistic origin in breast cancer.
format Online
Article
Text
id pubmed-10307628
institution National Center for Biotechnology Information
language English
publishDate 2023
publisher Nature Publishing Group UK
record_format MEDLINE/PubMed
spelling pubmed-103076282023-06-30 ERα-associated translocations underlie oncogene amplifications in breast cancer Lee, Jake June-Koo Jung, Youngsook Lucy Cheong, Taek-Chin Espejo Valle-Inclan, Jose Chu, Chong Gulhan, Doga C. Ljungström, Viktor Jin, Hu Viswanadham, Vinayak V. Watson, Emma V. Cortés-Ciriano, Isidro Elledge, Stephen J. Chiarle, Roberto Pellman, David Park, Peter J. Nature Article Focal copy-number amplification is an oncogenic event. Although recent studies have revealed the complex structure(1–3) and the evolutionary trajectories(4) of oncogene amplicons, their origin remains poorly understood. Here we show that focal amplifications in breast cancer frequently derive from a mechanism—which we term translocation–bridge amplification—involving inter-chromosomal translocations that lead to dicentric chromosome bridge formation and breakage. In 780 breast cancer genomes, we observe that focal amplifications are frequently connected to each other by inter-chromosomal translocations at their boundaries. Subsequent analysis indicates the following model: the oncogene neighbourhood is translocated in G1 creating a dicentric chromosome, the dicentric chromosome is replicated, and as dicentric sister chromosomes segregate during mitosis, a chromosome bridge is formed and then broken, with fragments often being circularized in extrachromosomal DNAs. This model explains the amplifications of key oncogenes, including ERBB2 and CCND1. Recurrent amplification boundaries and rearrangement hotspots correlate with oestrogen receptor binding in breast cancer cells. Experimentally, oestrogen treatment induces DNA double-strand breaks in the oestrogen receptor target regions that are repaired by translocations, suggesting a role of oestrogen in generating the initial translocations. A pan-cancer analysis reveals tissue-specific biases in mechanisms initiating focal amplifications, with the breakage–fusion–bridge cycle prevalent in some and the translocation–bridge amplification in others, probably owing to the different timing of DNA break repair. Our results identify a common mode of oncogene amplification and propose oestrogen as its mechanistic origin in breast cancer. Nature Publishing Group UK 2023-05-17 2023 /pmc/articles/PMC10307628/ /pubmed/37198482 http://dx.doi.org/10.1038/s41586-023-06057-w Text en © The Author(s) 2023 https://creativecommons.org/licenses/by/4.0/Open Access This article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons licence, and indicate if changes were made. The images or other third party material in this article are included in the article’s Creative Commons licence, unless indicated otherwise in a credit line to the material. If material is not included in the article’s Creative Commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder. To view a copy of this licence, visit http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Article
Lee, Jake June-Koo
Jung, Youngsook Lucy
Cheong, Taek-Chin
Espejo Valle-Inclan, Jose
Chu, Chong
Gulhan, Doga C.
Ljungström, Viktor
Jin, Hu
Viswanadham, Vinayak V.
Watson, Emma V.
Cortés-Ciriano, Isidro
Elledge, Stephen J.
Chiarle, Roberto
Pellman, David
Park, Peter J.
ERα-associated translocations underlie oncogene amplifications in breast cancer
title ERα-associated translocations underlie oncogene amplifications in breast cancer
title_full ERα-associated translocations underlie oncogene amplifications in breast cancer
title_fullStr ERα-associated translocations underlie oncogene amplifications in breast cancer
title_full_unstemmed ERα-associated translocations underlie oncogene amplifications in breast cancer
title_short ERα-associated translocations underlie oncogene amplifications in breast cancer
title_sort erα-associated translocations underlie oncogene amplifications in breast cancer
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10307628/
https://www.ncbi.nlm.nih.gov/pubmed/37198482
http://dx.doi.org/10.1038/s41586-023-06057-w
work_keys_str_mv AT leejakejunekoo eraassociatedtranslocationsunderlieoncogeneamplificationsinbreastcancer
AT jungyoungsooklucy eraassociatedtranslocationsunderlieoncogeneamplificationsinbreastcancer
AT cheongtaekchin eraassociatedtranslocationsunderlieoncogeneamplificationsinbreastcancer
AT espejovalleinclanjose eraassociatedtranslocationsunderlieoncogeneamplificationsinbreastcancer
AT chuchong eraassociatedtranslocationsunderlieoncogeneamplificationsinbreastcancer
AT gulhandogac eraassociatedtranslocationsunderlieoncogeneamplificationsinbreastcancer
AT ljungstromviktor eraassociatedtranslocationsunderlieoncogeneamplificationsinbreastcancer
AT jinhu eraassociatedtranslocationsunderlieoncogeneamplificationsinbreastcancer
AT viswanadhamvinayakv eraassociatedtranslocationsunderlieoncogeneamplificationsinbreastcancer
AT watsonemmav eraassociatedtranslocationsunderlieoncogeneamplificationsinbreastcancer
AT cortescirianoisidro eraassociatedtranslocationsunderlieoncogeneamplificationsinbreastcancer
AT elledgestephenj eraassociatedtranslocationsunderlieoncogeneamplificationsinbreastcancer
AT chiarleroberto eraassociatedtranslocationsunderlieoncogeneamplificationsinbreastcancer
AT pellmandavid eraassociatedtranslocationsunderlieoncogeneamplificationsinbreastcancer
AT parkpeterj eraassociatedtranslocationsunderlieoncogeneamplificationsinbreastcancer

Ejemplares similares