Tumor transcriptome-wide expression classifiers predict treatment sensitivity in advanced prostate cancers

Grist, Emily; Dutey-Magni, Peter; Parry, Marina A.; Mendes, Larissa; Sachdeva, Ashwin; Proudfoot, James A.; Hamid, Anis A.; Ismail, Mazlina; Howlett, Sarah; Friedrich, Stefanie; DePaula Oliveira, Lia; Murphy, Laura; Brawley, Christopher; Dairo, Oluwademilade; Lall, Sharanpreet; Liu, Yang; Wetterskog, Daniel; Wingate, Anna; Nowakowska, Karolina; Zakka, Leila; Amos, Claire L.; Atako, Nafisah B.; Wang, Victoria; Rush, Hannah L.; Jones, Robert J.; Leung, Hing; Cross, William R.; Gillessen, Silke; Parker, Chris C.; Marafioti, Teresa; Urbanucci, Alfonso; Fittall, Matthew; Schaeffer, Edward M.; Spratt, Daniel E.; Waugh, David; Powles, Thomas; Sydes, Matthew R.; Feng, Felix Y.; Berney, Daniel M.; Parmar, Mahesh K.B.; Clarke, Noel W.; Davicioni, Elai; Lotan, Tamara L.; Sweeney, Christopher J.; Brown, Louise C.; James, Nicholas D.; Attard, Gerhardt (2025)
 
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Grist, Emily
Dutey-Magni, Peter
Parry, Marina A.
Mendes, Larissa
Sachdeva, Ashwin
Proudfoot, James A.
Hamid, Anis A.
Ismail, Mazlina
Howlett, Sarah
Friedrich, Stefanie
DePaula Oliveira, Lia
Murphy, Laura
Brawley, Christopher
Dairo, Oluwademilade
Lall, Sharanpreet
Liu, Yang
Wetterskog, Daniel
Wingate, Anna
Nowakowska, Karolina
Zakka, Leila
Amos, Claire L.
Atako, Nafisah B.
Wang, Victoria
Rush, Hannah L.
Jones, Robert J.
Leung, Hing
Cross, William R.
Gillessen, Silke
Parker, Chris C.
Marafioti, Teresa
Urbanucci, Alfonso
Fittall, Matthew
Schaeffer, Edward M.
Spratt, Daniel E.
Waugh, David
Powles, Thomas
Sydes, Matthew R.
Feng, Felix Y.
Berney, Daniel M.
Parmar, Mahesh K.B.
Clarke, Noel W.
Davicioni, Elai
Lotan, Tamara L.
Sweeney, Christopher J.
Brown, Louise C.
James, Nicholas D.
Attard, Gerhardt
2025

Cell
doi:10.1016/j.cell.2025.07.042
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https://urn.fi/URN:NBN:fi:tuni-202510079713

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Peer reviewed
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Advanced prostate cancers respond to hormone therapy but outcomes vary and no predictive tests exist for informed treatment selection. To identify novel biomarker-treatment pairings, we examined associations between biological pathways and 14-year survival outcomes of patients randomized in practice-changing phase 3 trials (testing docetaxel or abiraterone). We included transcriptome-wide expression signatures and immunohistochemistry markers (Ki-67 and PTEN) on prostate tumors from 1,523 patients (832 metastatic). Tumor androgen receptor signaling is associated with longer survival, whereas increased proliferation predicted shorter survival. In a pre-specified analysis, the previously identified decipher RNA signature was both prognostic and predicted survival benefit from docetaxel for metastatic cancers (biomarker-docetaxel interaction p = 0.039). Additionally, transcriptome-based classification of PTEN inactivation identified tumors more likely to have PTEN protein loss (p = 4 × 10−37) and metabolically perturbed metastatic cancers that had shorter survival with hormone therapies (p < 0.001) but exhibited docetaxel sensitivity (biomarker-docetaxel interaction p = 0.002). Transcriptome classifiers predict docetaxel benefit and could be clinically implemented for improved patient management.
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