MCL-1 gains occur with high frequency in lung adenocarcinoma and can be targeted therapeutically

Enkhtsetseg Munkhbaatar,Michelle Dietzen,Deepti Agrawal,Martina Anton,Moritz Jesinghaus,Melanie Boxberg,Nicole Pfarr,Pidassa Bidola,Sebastian Uhrig,Ulrike Höckendorf,Anna-Lena Meinhardt,Adam Wahida,Irina Heid,Rickmer Braren,Ritu Mishra,Arne Warth,Thomas Muley,Patrina S. P. Poh,Xin Wang,Stefan Fröhling,Katja Steiger,Julia Slotta-Huspenina,Martijn van Griensven,Franz Pfeiffer,Sebastian Lange,Roland Rad,Magda Spella,Georgios T. Stathopoulos,Jürgen Ruland,Florian Bassermann,Wilko Weichert,Andreas Strasser,Caterina Branca,Mathias Heikenwalder,Charles Swanton,Nicholas McGranahan,Philipp J. Jost

MCL-1 gains occur with high frequency in lung adenocarcinoma and can be targeted therapeutically

2020

Evasion of programmed cell death represents a critical form of oncogene addiction in cancer cells. Understanding the molecular mechanisms underpinning cancer cell survival despite the oncogenic stress could provide a molecular basis for potential therapeutic interventions. Here we explore the role of pro-survival genes in cancer cell integrity during clonal evolution in non-small cell lung cancer (NSCLC). We identify gains of MCL-1 at high frequency in multiple independent NSCLC cohorts, occurring both clonally and subclonally. Clonal loss of functional TP53 is significantly associated with subclonal gains of MCL-1. In mice, tumour progression is delayed upon pharmacologic or genetic inhibition of MCL-1. These findings reveal that MCL-1 gains occur with high frequency in lung adenocarcinoma and can be targeted therapeutically.

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