Mapping extrachromosomal DNA amplifications during cancer progression

Hoon Kim; Soyeon Kim; Taylor Wade; Eunchae Yeo; Anuja Lipsa; Anna Golebiewska; Kevin C. Johnson; Sepil An; Junyong Ko; Yoonjoo Nam; Hwa Yeon Lee; Seunghyun Kang; Heesuk Chung; Simone P. Niclou; Hyo Eun Moon; Sun Ha Paek; Vineet Bafna; Jens Luebeck; Roel G.W. Verhaak

doi:10.1038/s41588-024-01949-7

Mapping extrachromosomal DNA amplifications during cancer progression

Hoon Kim
, Soyeon Kim
, Taylor Wade
, Eunchae Yeo
, Anuja Lipsa
, Anna Golebiewska
, Kevin C. Johnson
, Sepil An
, Junyong Ko
, Yoonjoo Nam
, Hwa Yeon Lee
, Seunghyun Kang
, Heesuk Chung
, Simone P. Niclou
, Hyo Eun Moon
, Sun Ha Paek
, Vineet Bafna
, Jens Luebeck
, Roel G.W. Verhaak

Department of Pharmacy

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

32 Scopus citations

Abstract

To understand the role of extrachromosomal DNA (ecDNA) amplifications in cancer progression, we detected and classified focal amplifications in 8,060 newly diagnosed primary cancers, untreated metastases and heavily pretreated tumors. The ecDNAs were detected at significantly higher frequency in untreated metastatic and pretreated tumors compared to newly diagnosed cancers. Tumors from chemotherapy-pretreated patients showed significantly higher ecDNA frequency compared to untreated cancers. In particular, tubulin inhibition associated with ecDNA increases, suggesting a role for ecDNA in treatment response. In longitudinally matched tumor samples, ecDNAs were more likely to be retained compared to chromosomal amplifications. EcDNAs shared between time points, and ecDNAs in advanced cancers were more likely to harbor localized hypermutation events compared to private ecDNAs and ecDNAs in newly diagnosed tumors. Relatively high variant allele fractions of ecDNA localized hypermutations implicated early ecDNA mutagenesis. Our findings nominate ecDNAs to provide tumors with competitive advantages during cancer progression and metastasis.

Original language	English
Pages (from-to)	2447-2454
Number of pages	8
Journal	Nature Genetics
Volume	56
Issue number	11
DOIs	https://doi.org/10.1038/s41588-024-01949-7
State	Published - Nov 2024

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Kim, H., Kim, S., Wade, T., Yeo, E., Lipsa, A., Golebiewska, A., Johnson, K. C., An, S., Ko, J., Nam, Y., Lee, H. Y., Kang, S., Chung, H., Niclou, S. P., Moon, H. E., Paek, S. H., Bafna, V., Luebeck, J., & Verhaak, R. G. W. (2024). Mapping extrachromosomal DNA amplifications during cancer progression. Nature Genetics, 56(11), 2447-2454. https://doi.org/10.1038/s41588-024-01949-7

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title = "Mapping extrachromosomal DNA amplifications during cancer progression",

abstract = "To understand the role of extrachromosomal DNA (ecDNA) amplifications in cancer progression, we detected and classified focal amplifications in 8,060 newly diagnosed primary cancers, untreated metastases and heavily pretreated tumors. The ecDNAs were detected at significantly higher frequency in untreated metastatic and pretreated tumors compared to newly diagnosed cancers. Tumors from chemotherapy-pretreated patients showed significantly higher ecDNA frequency compared to untreated cancers. In particular, tubulin inhibition associated with ecDNA increases, suggesting a role for ecDNA in treatment response. In longitudinally matched tumor samples, ecDNAs were more likely to be retained compared to chromosomal amplifications. EcDNAs shared between time points, and ecDNAs in advanced cancers were more likely to harbor localized hypermutation events compared to private ecDNAs and ecDNAs in newly diagnosed tumors. Relatively high variant allele fractions of ecDNA localized hypermutations implicated early ecDNA mutagenesis. Our findings nominate ecDNAs to provide tumors with competitive advantages during cancer progression and metastasis.",

author = "Hoon Kim and Soyeon Kim and Taylor Wade and Eunchae Yeo and Anuja Lipsa and Anna Golebiewska and Johnson, \{Kevin C.\} and Sepil An and Junyong Ko and Yoonjoo Nam and Lee, \{Hwa Yeon\} and Seunghyun Kang and Heesuk Chung and Niclou, \{Simone P.\} and Moon, \{Hyo Eun\} and Paek, \{Sun Ha\} and Vineet Bafna and Jens Luebeck and Verhaak, \{Roel G.W.\}",

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doi = "10.1038/s41588-024-01949-7",

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AU - Golebiewska, Anna

AU - Johnson, Kevin C.

AU - An, Sepil

AU - Ko, Junyong

AU - Nam, Yoonjoo

AU - Lee, Hwa Yeon

AU - Kang, Seunghyun

AU - Chung, Heesuk

AU - Niclou, Simone P.

AU - Moon, Hyo Eun

AU - Paek, Sun Ha

AU - Bafna, Vineet

AU - Luebeck, Jens

AU - Verhaak, Roel G.W.

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N2 - To understand the role of extrachromosomal DNA (ecDNA) amplifications in cancer progression, we detected and classified focal amplifications in 8,060 newly diagnosed primary cancers, untreated metastases and heavily pretreated tumors. The ecDNAs were detected at significantly higher frequency in untreated metastatic and pretreated tumors compared to newly diagnosed cancers. Tumors from chemotherapy-pretreated patients showed significantly higher ecDNA frequency compared to untreated cancers. In particular, tubulin inhibition associated with ecDNA increases, suggesting a role for ecDNA in treatment response. In longitudinally matched tumor samples, ecDNAs were more likely to be retained compared to chromosomal amplifications. EcDNAs shared between time points, and ecDNAs in advanced cancers were more likely to harbor localized hypermutation events compared to private ecDNAs and ecDNAs in newly diagnosed tumors. Relatively high variant allele fractions of ecDNA localized hypermutations implicated early ecDNA mutagenesis. Our findings nominate ecDNAs to provide tumors with competitive advantages during cancer progression and metastasis.

AB - To understand the role of extrachromosomal DNA (ecDNA) amplifications in cancer progression, we detected and classified focal amplifications in 8,060 newly diagnosed primary cancers, untreated metastases and heavily pretreated tumors. The ecDNAs were detected at significantly higher frequency in untreated metastatic and pretreated tumors compared to newly diagnosed cancers. Tumors from chemotherapy-pretreated patients showed significantly higher ecDNA frequency compared to untreated cancers. In particular, tubulin inhibition associated with ecDNA increases, suggesting a role for ecDNA in treatment response. In longitudinally matched tumor samples, ecDNAs were more likely to be retained compared to chromosomal amplifications. EcDNAs shared between time points, and ecDNAs in advanced cancers were more likely to harbor localized hypermutation events compared to private ecDNAs and ecDNAs in newly diagnosed tumors. Relatively high variant allele fractions of ecDNA localized hypermutations implicated early ecDNA mutagenesis. Our findings nominate ecDNAs to provide tumors with competitive advantages during cancer progression and metastasis.

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VL - 56

SP - 2447

EP - 2454

JO - Nature Genetics

JF - Nature Genetics

IS - 11

ER -

Mapping extrachromosomal DNA amplifications during cancer progression

Abstract

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