Drug-resilient cancer cell phenotype is acquired via polyploidization associated with early stress response coupled to HIF-2α transcriptional regulation

Christopher Carroll; Auraya Manaprasertsak; Arthur Boffelli Castro; Hilda van den Bos; Diana C J Spierings; René Wardenaar; Anuraag Bukkuri; Niklas Engström; Etienne Baratchart; Minjun Yang; Andrea Biloglav; Charlie Cornwallis; Bertil Johansson; Catharina Hagerling; Marie Arsenian-Henriksson; Kajsa Paulsson; Sarah R Amend; Sofie Mohlin; Floris Foijer; Alan McIntyre; Kenneth J Pienta; Emma U Hammarlund

doi:10.1158/2767-9764.CRC-23-0396

Drug-resilient cancer cell phenotype is acquired via polyploidization associated with early stress response coupled to HIF-2α transcriptional regulation

Christopher Carroll, Auraya Manaprasertsak, Arthur Boffelli Castro, Hilda van den Bos, Diana C J Spierings, René Wardenaar, Anuraag Bukkuri, Niklas Engström, Etienne Baratchart, Minjun Yang, Andrea Biloglav, Charlie Cornwallis, Bertil Johansson, Catharina Hagerling, Marie Arsenian-Henriksson, Kajsa Paulsson, Sarah R Amend, Sofie Mohlin, Floris Foijer, Alan McIntyreKenneth J Pienta, Emma U Hammarlund

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Therapeutic resistance and recurrence remain core challenges in cancer therapy. How therapy resistance arises is currently not fully understood with tumors surviving via multiple alternative routes. Here, we demonstrate that a subset of cancer cells survives therapeutic stress by entering a transient state characterized by whole genome doubling. At the onset of the polyploidization program, we identified an upregulation of key transcriptional regulators, including the early stress-response protein AP-1 and normoxic stabilization of HIF-2α. We found altered chromatin accessibility, ablated expression of RB1, and enrichment of AP-1 motif accessibility. We demonstrate that AP-1 and HIF-2α regulate a therapy resilient and survivor phenotype in cancer cells. Consistent with this, genetic or pharmacologic targeting of AP-1 and HIF-2α reduced the number of surviving cells following chemotherapy treatment. The role of AP-1 and HIF-2α in stress-response by polyploidy suggest a novel avenue for tackling chemotherapy-induced resistance in cancer.

Originele taal-2	English
Pagina's (van-tot)	691–705
Aantal pagina's	15
Tijdschrift	Cancer research communications
Volume	4
Nummer van het tijdschrift	3
Vroegere onlinedatum	22-feb.-2024
DOI's	https://doi.org/10.1158/2767-9764.CRC-23-0396
Status	Published - 7-mrt.-2024

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10.1158/2767-9764.CRC-23-0396Licentie: CC BY

Drug-resilient Cancer Cell Phenotype Is Acquired via Polyploidization Associated with Early Stress ResponseFinal publisher's version, 11,3 MBLicentie: CC BY

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Carroll, C., Manaprasertsak, A., Boffelli Castro, A., van den Bos, H., Spierings, D. C. J., Wardenaar, R., Bukkuri, A., Engström, N., Baratchart, E., Yang, M., Biloglav, A., Cornwallis, C., Johansson, B., Hagerling, C., Arsenian-Henriksson, M., Paulsson, K., Amend, S. R., Mohlin, S., Foijer, F., ... Hammarlund, E. U. (2024). Drug-resilient cancer cell phenotype is acquired via polyploidization associated with early stress response coupled to HIF-2α transcriptional regulation. Cancer research communications, 4(3), 691–705. https://doi.org/10.1158/2767-9764.CRC-23-0396

@article{eb03c057b06e44d0b2da9838c662f40a,

title = "Drug-resilient cancer cell phenotype is acquired via polyploidization associated with early stress response coupled to HIF-2α transcriptional regulation",

abstract = "Therapeutic resistance and recurrence remain core challenges in cancer therapy. How therapy resistance arises is currently not fully understood with tumors surviving via multiple alternative routes. Here, we demonstrate that a subset of cancer cells survives therapeutic stress by entering a transient state characterized by whole genome doubling. At the onset of the polyploidization program, we identified an upregulation of key transcriptional regulators, including the early stress-response protein AP-1 and normoxic stabilization of HIF-2α. We found altered chromatin accessibility, ablated expression of RB1, and enrichment of AP-1 motif accessibility. We demonstrate that AP-1 and HIF-2α regulate a therapy resilient and survivor phenotype in cancer cells. Consistent with this, genetic or pharmacologic targeting of AP-1 and HIF-2α reduced the number of surviving cells following chemotherapy treatment. The role of AP-1 and HIF-2α in stress-response by polyploidy suggest a novel avenue for tackling chemotherapy-induced resistance in cancer.",

author = "Christopher Carroll and Auraya Manaprasertsak and {Boffelli Castro}, Arthur and {van den Bos}, Hilda and Spierings, {Diana C J} and Ren{\'e} Wardenaar and Anuraag Bukkuri and Niklas Engstr{\"o}m and Etienne Baratchart and Minjun Yang and Andrea Biloglav and Charlie Cornwallis and Bertil Johansson and Catharina Hagerling and Marie Arsenian-Henriksson and Kajsa Paulsson and Amend, {Sarah R} and Sofie Mohlin and Floris Foijer and Alan McIntyre and Pienta, {Kenneth J} and Hammarlund, {Emma U}",

year = "2024",

month = mar,

day = "7",

doi = "10.1158/2767-9764.CRC-23-0396",

language = "English",

volume = "4",

pages = "691–705",

journal = "Cancer research communications",

issn = "2767-9764",

publisher = "American Association for Cancer Research Inc.",

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Carroll, C, Manaprasertsak, A, Boffelli Castro, A, van den Bos, H, Spierings, DCJ , Wardenaar, R, Bukkuri, A, Engström, N, Baratchart, E, Yang, M, Biloglav, A, Cornwallis, C, Johansson, B, Hagerling, C, Arsenian-Henriksson, M, Paulsson, K, Amend, SR, Mohlin, S, Foijer, F, McIntyre, A, Pienta, KJ & Hammarlund, EU 2024, 'Drug-resilient cancer cell phenotype is acquired via polyploidization associated with early stress response coupled to HIF-2α transcriptional regulation', Cancer research communications, vol. 4, nr. 3, blz. 691–705. https://doi.org/10.1158/2767-9764.CRC-23-0396

TY - JOUR

T1 - Drug-resilient cancer cell phenotype is acquired via polyploidization associated with early stress response coupled to HIF-2α transcriptional regulation

AU - Carroll, Christopher

AU - Manaprasertsak, Auraya

AU - Boffelli Castro, Arthur

AU - van den Bos, Hilda

AU - Spierings, Diana C J

AU - Wardenaar, René

AU - Bukkuri, Anuraag

AU - Engström, Niklas

AU - Baratchart, Etienne

AU - Yang, Minjun

AU - Biloglav, Andrea

AU - Cornwallis, Charlie

AU - Johansson, Bertil

AU - Hagerling, Catharina

AU - Arsenian-Henriksson, Marie

AU - Paulsson, Kajsa

AU - Amend, Sarah R

AU - Mohlin, Sofie

AU - Foijer, Floris

AU - McIntyre, Alan

AU - Pienta, Kenneth J

AU - Hammarlund, Emma U

PY - 2024/3/7

Y1 - 2024/3/7

N2 - Therapeutic resistance and recurrence remain core challenges in cancer therapy. How therapy resistance arises is currently not fully understood with tumors surviving via multiple alternative routes. Here, we demonstrate that a subset of cancer cells survives therapeutic stress by entering a transient state characterized by whole genome doubling. At the onset of the polyploidization program, we identified an upregulation of key transcriptional regulators, including the early stress-response protein AP-1 and normoxic stabilization of HIF-2α. We found altered chromatin accessibility, ablated expression of RB1, and enrichment of AP-1 motif accessibility. We demonstrate that AP-1 and HIF-2α regulate a therapy resilient and survivor phenotype in cancer cells. Consistent with this, genetic or pharmacologic targeting of AP-1 and HIF-2α reduced the number of surviving cells following chemotherapy treatment. The role of AP-1 and HIF-2α in stress-response by polyploidy suggest a novel avenue for tackling chemotherapy-induced resistance in cancer.

AB - Therapeutic resistance and recurrence remain core challenges in cancer therapy. How therapy resistance arises is currently not fully understood with tumors surviving via multiple alternative routes. Here, we demonstrate that a subset of cancer cells survives therapeutic stress by entering a transient state characterized by whole genome doubling. At the onset of the polyploidization program, we identified an upregulation of key transcriptional regulators, including the early stress-response protein AP-1 and normoxic stabilization of HIF-2α. We found altered chromatin accessibility, ablated expression of RB1, and enrichment of AP-1 motif accessibility. We demonstrate that AP-1 and HIF-2α regulate a therapy resilient and survivor phenotype in cancer cells. Consistent with this, genetic or pharmacologic targeting of AP-1 and HIF-2α reduced the number of surviving cells following chemotherapy treatment. The role of AP-1 and HIF-2α in stress-response by polyploidy suggest a novel avenue for tackling chemotherapy-induced resistance in cancer.

U2 - 10.1158/2767-9764.CRC-23-0396

DO - 10.1158/2767-9764.CRC-23-0396

M3 - Article

C2 - 38385626

SN - 2767-9764

VL - 4

SP - 691

EP - 705

JO - Cancer research communications

JF - Cancer research communications

IS - 3

ER -

Drug-resilient cancer cell phenotype is acquired via polyploidization associated with early stress response coupled to HIF-2α transcriptional regulation

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