Mixed responses to targeted therapy driven by chromosomal instability through p53 dysfunction and genome doubling
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Published:2024-06-13
Issue:1
Volume:15
Page:
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ISSN:2041-1723
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Container-title:Nature Communications
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language:en
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Short-container-title:Nat Commun
Author:
Hobor Sebastijan, Al Bakir MaiseORCID, Hiley Crispin T., Skrzypski Marcin, Frankell Alexander M.ORCID, Bakker Bjorn, Watkins Thomas B. K., Markovets Aleksandra, Dry Jonathan R.ORCID, Brown Andrew P., van der Aart JasperORCID, van den Bos Hilda, Spierings DianaORCID, Oukrif Dahmane, Novelli Marco, Chakrabarti Turja, Rabinowitz Adam H., Ait Hassou Laila, Litière Saskia, Kerr D. LucasORCID, Tan Lisa, Kelly GavinORCID, Moore David A.ORCID, Renshaw Matthew J.ORCID, Venkatesan Subramanian, Hill William, Huebner ArianaORCID, Martínez-Ruiz CarlosORCID, Black James R. M.ORCID, Wu WeiORCID, Angelova MihaelaORCID, McGranahan NicholasORCID, Downward JulianORCID, Chmielecki Juliann, Barrett Carl, Litchfield KevinORCID, Chew Su Kit, Blakely Collin M.ORCID, de Bruin Elza C.ORCID, Foijer Floris, Vousden Karen H.ORCID, Bivona Trever G.ORCID, , Lester Jason F., Bajaj Amrita, Nakas Apostolos, Sodha-Ramdeen Azmina, Tufail Mohamad, Scotland Molly, Boyles Rebecca, Rathinam Sridhar, Wilson Claire, Marrone Domenic, Dulloo Sean, Fennell Dean A., Matharu Gurdeep, Shaw Jacqui A., Boleti Ekaterini, Cheyne Heather, Khalil Mohammed, Richardson Shirley, Cruickshank Tracey, Price Gillian, Kerr Keith M., Benafif Sarah, French Jack, Gilbert Kayleigh, Naidu Babu, Patel Akshay J., Osman Aya, Enstone Carol, Langman Gerald, Shackleford Helen, Djearaman Madava, Kadiri Salma, Middleton Gary, Leek Angela, Hodgkinson Jack Davies, Totton Nicola, Montero Angeles, Smith Elaine, Fontaine Eustace, Granato Felice, Paiva-Correia Antonio, Novasio Juliette, Rammohan Kendadai, Joseph Leena, Bishop Paul, Shah Rajesh, Moss Stuart, Joshi Vijay, Crosbie Philip A. J., Brown Katherine D., Carter Mathew, Chaturvedi Anshuman, Oliveira Pedro, Lindsay Colin R., Blackhall Fiona H., Krebs Matthew G., Summers Yvonne, Clipson Alexandra, Tugwood Jonathan, Kerr Alastair, Rothwell Dominic G., Dive Caroline, Aerts Hugo J. W. L., Schwarz Roland F., Kaufmann Tom L., Wilson Gareth A., Rosenthal Rachel, Van Loo Peter, Birkbak Nicolai J., Szallasi Zoltan, Kisistok Judit, Sokac Mateo, Salgado Roberto, Diossy Miklos, Demeulemeester Jonas, Bunkum Abigail, Dwornik Angela, Magness Alastair, Rowan Andrew J., Karamani Angeliki, Toncheva Antonia, Chain Benny, Castignani Carla, Bailey Chris, Abbosh Christopher, Puttick Clare, Weeden Clare E., Lee Claudia, Richard Corentin, Naceur-Lombardelli Cristina, Pearce David R., Karagianni Despoina, Biswas Dhruva, Levi Dina, Larose Cadieux Elizabeth, Lim Emilia L., Colliver Emma, Nye Emma, Gálvez-Cancino Felip, Gimeno-Valiente Francisco, Kassiotis George, Stavrou Georgia, Mastrokalos Gerasimos-Theodoros, Lowe Helen L., Matos Ignacio Garcia, Noorani Imran, Goldman Jacki, Reading James L., Rane Jayant K., Nicod Jerome, Hartley John A., Peggs Karl S., Enfield Katey S. S., Selvaraju Kayalvizhi, Thol Kerstin, Ng Kevin W., Chen Kezhong, Dijkstra Krijn, Grigoriadis Kristiana, Thakkar Krupa, Ensell Leah, Shah Mansi, Litovchenko Maria, Jamal-Hanjani Mariam, Werner Sunderland Mariana, Huska Matthew R., Hill Mark S., Dietzen Michelle, Leung Michelle M., Escudero Mickael, Tanić Miljana, Sivakumar Monica, Chervova Olga, Lucas Olivia, Pich Oriol, Al-Sawaf Othman, Prymas Paulina, Hobson Philip, Pawlik Piotr, Stone Richard Kevin, Bentham Robert, Vendramin Roberto, Saghafinia Sadegh, Gamble Samuel, Veeriah Selvaraju, Ung Seng Kuong Anakin, Quezada Sergio A., Vanloo Sharon, Hessey Sonya, Ward Sophia, Harries Sian, Boeing Stefan, Beck Stephan, Bola Supreet Kaur, Karasaki Takahiro, Denner Tamara, Marafioti Teresa, Jones Thomas Patrick, Spanswick Victoria, Barbè Vittorio, Lu Wei-Ting, Liu Wing Kin, Wu Yin, Naito Yutaka, Ramsden Zoe, Veiga Catarina, Royle Gary, Collins-Fekete Charles-Antoine, Fraioli Francesco, Ashford Paul, Forster Martin D., Lee Siow Ming, Borg Elaine, Falzon Mary, Papadatos-Pastos Dionysis, Wilson James, Ahmad Tanya, Procter Alexander James, Ahmed Asia, Taylor Magali N., Nair Arjun, Lawrence David, Patrini Davide, Navani Neal, Thakrar Ricky M., Janes Sam M., Martinoni Hoogenboom Emilie, Monk Fleur, Holding James W., Choudhary Junaid, Bhakhri Kunal, Scarci Marco, Gorman Pat, Khiroya Reena, Stephens Robert C. M., Wong Yien Ning Sophia, Kaplar Zoltan, Bandula Steve, Hackshaw Allan, Hacker Anne-Marie, Sharp Abigail, Smith Sean, Kaur Dhanda Harjot, Pilotti Camilla, Leslie Rachel, Grapa Anca, Zhang Hanyun, AbdulJabbar Khalid, Pan Xiaoxi, Yuan Yinyin, Chuter David, MacKenzie Mairead, Chee Serena, Alzetani Aiman, Cave Judith, Richards Jennifer, Lim Eric, De Sousa Paulo, Jordan Simon, Rice Alexandra, Raubenheimer Hilgardt, Bhayani Harshil, Ambrose Lyn, Devaraj Anand, Chavan Hema, Begum Sofina, Buderi Silviu I., Kaniu Daniel, Malima Mpho, Booth Sarah, Nicholson Andrew G., Fernandes Nadia, Shah Pratibha, Proli Chiara, Hewish Madeleine, Danson Sarah, Shackcloth Michael J., Robinson Lily, Russell Peter, Blyth Kevin G., Kidd Andrew, Dick Craig, Le Quesne John, Kirk Alan, Asif Mo, Bilancia Rocco, Kostoulas Nikos, Thomas Mathew, Hynds Robert E.ORCID, Kanu Nnennaya, Zaccaria SimoneORCID, Grönroos EvaORCID, Swanton CharlesORCID
Abstract
AbstractThe 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.
Publisher
Springer Science and Business Media LLC
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