Mixed responses to targeted therapy driven by chromosomal instability through p53 dysfunction and genome doubling

TRACERx consortium; Sebastijan Hobor; Maise Al Bakir; Crispin T Hiley; Marcin Skrzypski; Alexander M Frankell; Bjorn Bakker; Thomas B K Watkins; Aleksandra Markovets; Jonathan R Dry; Andrew P Brown; Jasper van der Aart; Hilda van den Bos; Diana Spierings; Dahmane Oukrif; Marco Novelli; Turja Chakrabarti; Adam H Rabinowitz; Laila Ait Hassou; Saskia Litière; D Lucas Kerr; Lisa Tan; Gavin Kelly; David A Moore; Matthew J Renshaw; Subramanian Venkatesan; William Hill; Ariana Huebner; Carlos Martínez-Ruiz; James R M Black; Wei Wu; Mihaela Angelova; Nicholas McGranahan; Julian Downward; Juliann Chmielecki; Carl Barrett; Kevin Litchfield; Su Kit Chew; Collin M Blakely; Elza C de Bruin; Floris Foijer; Karen H Vousden; Trever G Bivona; Robert E Hynds; Nnennaya Kanu; Simone Zaccaria; Eva Grönroos; Charles Swanton

doi:10.1038/s41467-024-47606-9

Mixed responses to targeted therapy driven by chromosomal instability through p53 dysfunction and genome doubling

TRACERx consortium, Sebastijan Hobor, Maise Al Bakir, Crispin T Hiley, Marcin Skrzypski, Alexander M Frankell, Bjorn Bakker, Thomas B K Watkins, Aleksandra Markovets, Jonathan R Dry, Andrew P Brown, Jasper van der Aart, Hilda van den Bos, Diana Spierings, Dahmane Oukrif, Marco Novelli, Turja Chakrabarti, Adam H Rabinowitz, Laila Ait Hassou, Saskia LitièreD Lucas Kerr, Lisa Tan, Gavin Kelly, David A Moore, Matthew J Renshaw, Subramanian Venkatesan, William Hill, Ariana Huebner, Carlos Martínez-Ruiz, James R M Black, Wei Wu, Mihaela Angelova, Nicholas McGranahan, Julian Downward, Juliann Chmielecki, Carl Barrett, Kevin Litchfield, Su Kit Chew, Collin M Blakely, Elza C de Bruin, Floris Foijer, Karen H Vousden, Trever G Bivona, Robert E Hynds, Nnennaya Kanu, Simone Zaccaria, Eva Grönroos, Charles Swanton

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The phenomenon of mixed/heterogenous treatment responses to cancer therapies within an individual patient presents a challenging clinical scenario. Furthermore, the molecular basis of mixed intra-patient tumor responses remains unclear. Here, we show that patients with metastatic lung adenocarcinoma harbouring co-mutations of EGFR and TP53, are more likely to have mixed intra-patient tumor responses to EGFR tyrosine kinase inhibition (TKI), compared to those with an EGFR mutation alone. The combined presence of whole genome doubling (WGD) and TP53 co-mutations leads to increased genome instability and genomic copy number aberrations in genes implicated in EGFR TKI resistance. Using mouse models and an in vitro isogenic p53-mutant model system, we provide evidence that WGD provides diverse routes to drug resistance by increasing the probability of acquiring copy-number gains or losses relative to non-WGD cells. These data provide a molecular basis for mixed tumor responses to targeted therapy, within an individual patient, with implications for therapeutic strategies.

Originele taal-2	English
Artikelnummer	4871
Aantal pagina's	21
Tijdschrift	Nature Communications
Volume	15
Nummer van het tijdschrift	1
Vroegere onlinedatum	13-jun.-2024
DOI's	https://doi.org/10.1038/s41467-024-47606-9
Status	Published - 2024

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10.1038/s41467-024-47606-9Licentie: CC BY

Mixed responses to targeted therapy driven by chromosomal instability through p53 dysfunction and genome doublingFinal publisher's version, 3,12 MBLicentie: CC BY

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TRACERx consortium, Hobor, S., Al Bakir, M., Hiley, C. T., Skrzypski, M., Frankell, A. M., Bakker, B., Watkins, T. B. K., Markovets, A., Dry, J. R., Brown, A. P., van der Aart, J., van den Bos, H., Spierings, D., Oukrif, D., Novelli, M., Chakrabarti, T., Rabinowitz, A. H., Ait Hassou, L., ... Swanton, C. (2024). Mixed responses to targeted therapy driven by chromosomal instability through p53 dysfunction and genome doubling. Nature Communications, 15(1), Artikel 4871. https://doi.org/10.1038/s41467-024-47606-9

@article{38b9659673c54c15b9653b7f9c8e86b4,

title = "Mixed responses to targeted therapy driven by chromosomal instability through p53 dysfunction and genome doubling",

abstract = "The phenomenon of mixed/heterogenous treatment responses to cancer therapies within an individual patient presents a challenging clinical scenario. Furthermore, the molecular basis of mixed intra-patient tumor responses remains unclear. Here, we show that patients with metastatic lung adenocarcinoma harbouring co-mutations of EGFR and TP53, are more likely to have mixed intra-patient tumor responses to EGFR tyrosine kinase inhibition (TKI), compared to those with an EGFR mutation alone. The combined presence of whole genome doubling (WGD) and TP53 co-mutations leads to increased genome instability and genomic copy number aberrations in genes implicated in EGFR TKI resistance. Using mouse models and an in vitro isogenic p53-mutant model system, we provide evidence that WGD provides diverse routes to drug resistance by increasing the probability of acquiring copy-number gains or losses relative to non-WGD cells. These data provide a molecular basis for mixed tumor responses to targeted therapy, within an individual patient, with implications for therapeutic strategies.",

keywords = "Humans, Tumor Suppressor Protein p53/genetics, Animals, Chromosomal Instability, Mice, Lung Neoplasms/genetics, ErbB Receptors/genetics, Mutation, Drug Resistance, Neoplasm/genetics, Cell Line, Tumor, Protein Kinase Inhibitors/pharmacology, Adenocarcinoma of Lung/genetics, Molecular Targeted Therapy/methods, Female, DNA Copy Number Variations, Male",

author = "\{TRACERx consortium\} and Sebastijan Hobor and \{Al Bakir\}, Maise and Hiley, \{Crispin T\} and Marcin Skrzypski and Frankell, \{Alexander M\} and Bjorn Bakker and Watkins, \{Thomas B K\} and Aleksandra Markovets and Dry, \{Jonathan R\} and Brown, \{Andrew P\} and \{van der Aart\}, Jasper and \{van den Bos\}, Hilda and Diana Spierings and Dahmane Oukrif and Marco Novelli and Turja Chakrabarti and Rabinowitz, \{Adam H\} and \{Ait Hassou\}, Laila and Saskia Liti{\`e}re and Kerr, \{D Lucas\} and Lisa Tan and Gavin Kelly and Moore, \{David A\} and Renshaw, \{Matthew J\} and Subramanian Venkatesan and William Hill and Ariana Huebner and Carlos Mart{\'i}nez-Ruiz and Black, \{James R M\} and Wei Wu and Mihaela Angelova and Nicholas McGranahan and Julian Downward and Juliann Chmielecki and Carl Barrett and Kevin Litchfield and Chew, \{Su Kit\} and Blakely, \{Collin M\} and \{de Bruin\}, \{Elza C\} and Floris Foijer and Vousden, \{Karen H\} and Bivona, \{Trever G\} and Hynds, \{Robert E\} and Nnennaya Kanu and Simone Zaccaria and Eva Gr{\"o}nroos and Charles Swanton",

note = "{\textcopyright} 2024. The Author(s).",

year = "2024",

doi = "10.1038/s41467-024-47606-9",

language = "English",

volume = "15",

journal = "Nature Communications",

issn = "2041-1723",

publisher = "Nature Publishing Group",

number = "1",

}

TRACERx consortium, Hobor, S, Al Bakir, M, Hiley, CT, Skrzypski, M, Frankell, AM, Bakker, B, Watkins, TBK, Markovets, A, Dry, JR, Brown, AP, van der Aart, J, van den Bos, H, Spierings, D, Oukrif, D, Novelli, M, Chakrabarti, T, Rabinowitz, AH, Ait Hassou, L, Litière, S, Kerr, DL, Tan, L, Kelly, G, Moore, DA, Renshaw, MJ, Venkatesan, S, Hill, W, Huebner, A, Martínez-Ruiz, C, Black, JRM, Wu, W, Angelova, M, McGranahan, N, Downward, J, Chmielecki, J, Barrett, C, Litchfield, K, Chew, SK, Blakely, CM, de Bruin, EC, Foijer, F, Vousden, KH, Bivona, TG, Hynds, RE, Kanu, N, Zaccaria, S, Grönroos, E & Swanton, C 2024, 'Mixed responses to targeted therapy driven by chromosomal instability through p53 dysfunction and genome doubling', Nature Communications, vol. 15, nr. 1, 4871. https://doi.org/10.1038/s41467-024-47606-9

TY - JOUR

T1 - Mixed responses to targeted therapy driven by chromosomal instability through p53 dysfunction and genome doubling

AU - TRACERx consortium

AU - Hobor, Sebastijan

AU - Al Bakir, Maise

AU - Hiley, Crispin T

AU - Skrzypski, Marcin

AU - Frankell, Alexander M

AU - Bakker, Bjorn

AU - Watkins, Thomas B K

AU - Markovets, Aleksandra

AU - Dry, Jonathan R

AU - Brown, Andrew P

AU - van der Aart, Jasper

AU - van den Bos, Hilda

AU - Spierings, Diana

AU - Oukrif, Dahmane

AU - Novelli, Marco

AU - Chakrabarti, Turja

AU - Rabinowitz, Adam H

AU - Ait Hassou, Laila

AU - Litière, Saskia

AU - Kerr, D Lucas

AU - Tan, Lisa

AU - Kelly, Gavin

AU - Moore, David A

AU - Renshaw, Matthew J

AU - Venkatesan, Subramanian

AU - Hill, William

AU - Huebner, Ariana

AU - Martínez-Ruiz, Carlos

AU - Black, James R M

AU - Wu, Wei

AU - Angelova, Mihaela

AU - McGranahan, Nicholas

AU - Downward, Julian

AU - Chmielecki, Juliann

AU - Barrett, Carl

AU - Litchfield, Kevin

AU - Chew, Su Kit

AU - Blakely, Collin M

AU - de Bruin, Elza C

AU - Foijer, Floris

AU - Vousden, Karen H

AU - Bivona, Trever G

AU - Hynds, Robert E

AU - Kanu, Nnennaya

AU - Zaccaria, Simone

AU - Grönroos, Eva

AU - Swanton, Charles

PY - 2024

Y1 - 2024

N2 - The phenomenon of mixed/heterogenous treatment responses to cancer therapies within an individual patient presents a challenging clinical scenario. Furthermore, the molecular basis of mixed intra-patient tumor responses remains unclear. Here, we show that patients with metastatic lung adenocarcinoma harbouring co-mutations of EGFR and TP53, are more likely to have mixed intra-patient tumor responses to EGFR tyrosine kinase inhibition (TKI), compared to those with an EGFR mutation alone. The combined presence of whole genome doubling (WGD) and TP53 co-mutations leads to increased genome instability and genomic copy number aberrations in genes implicated in EGFR TKI resistance. Using mouse models and an in vitro isogenic p53-mutant model system, we provide evidence that WGD provides diverse routes to drug resistance by increasing the probability of acquiring copy-number gains or losses relative to non-WGD cells. These data provide a molecular basis for mixed tumor responses to targeted therapy, within an individual patient, with implications for therapeutic strategies.

AB - The phenomenon of mixed/heterogenous treatment responses to cancer therapies within an individual patient presents a challenging clinical scenario. Furthermore, the molecular basis of mixed intra-patient tumor responses remains unclear. Here, we show that patients with metastatic lung adenocarcinoma harbouring co-mutations of EGFR and TP53, are more likely to have mixed intra-patient tumor responses to EGFR tyrosine kinase inhibition (TKI), compared to those with an EGFR mutation alone. The combined presence of whole genome doubling (WGD) and TP53 co-mutations leads to increased genome instability and genomic copy number aberrations in genes implicated in EGFR TKI resistance. Using mouse models and an in vitro isogenic p53-mutant model system, we provide evidence that WGD provides diverse routes to drug resistance by increasing the probability of acquiring copy-number gains or losses relative to non-WGD cells. These data provide a molecular basis for mixed tumor responses to targeted therapy, within an individual patient, with implications for therapeutic strategies.

KW - Humans

KW - Tumor Suppressor Protein p53/genetics

KW - Animals

KW - Chromosomal Instability

KW - Mice

KW - Lung Neoplasms/genetics

KW - ErbB Receptors/genetics

KW - Mutation

KW - Drug Resistance, Neoplasm/genetics

KW - Cell Line, Tumor

KW - Protein Kinase Inhibitors/pharmacology

KW - Adenocarcinoma of Lung/genetics

KW - Molecular Targeted Therapy/methods

KW - Female

KW - DNA Copy Number Variations

KW - Male

U2 - 10.1038/s41467-024-47606-9

DO - 10.1038/s41467-024-47606-9

M3 - Article

C2 - 38871738

SN - 2041-1723

VL - 15

JO - Nature Communications

JF - Nature Communications

IS - 1

M1 - 4871

ER -

Mixed responses to targeted therapy driven by chromosomal instability through p53 dysfunction and genome doubling

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