SPOP-mutant prostate cancer: Translating fundamental biology into patient care

被引:19
作者
Bernasocchi, Tiziano [1 ,2 ]
Theurillat, Jean-Philippe P. [1 ,2 ]
机构
[1] Inst Oncol Res, CH-6500 Bellinzona, TI, Switzerland
[2] Univ Svizzera Italiana USI, Fac Biomed Sci, TI, CH-6900 Lugano, Switzerland
来源
CANCER LETTERS | 2022年 / 529卷
基金
瑞士国家科学基金会;
关键词
Prostate cancer; SPOP; Point mutations; Androgen receptor signaling; TRIM24; SRC-3; AR; DNA damage Repair; BRCAness; TUMOR-SUPPRESSOR SPOP; WILD-TYPE SPOP; ANDROGEN RECEPTOR; UBIQUITIN LIGASE; PROMOTES UBIQUITINATION; LINEAGE PLASTICITY; POZ PROTEIN; DEGRADATION; MUTATIONS; TRIM24;
D O I
10.1016/j.canlet.2021.12.024
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Comprehensive cancer genome studies have revealed genetically-defined subtypes of prostate cancer with distinct truncal driver mutations. Because prostate cancer has been largely seen as a rather uniform disease, the clinical significance of this discovery remained largely obscure. However, recent findings imply distinct biological features and therapeutic vulnerabilities linked to specific truncal mutations. Here we review our current understanding of prostate cancers harboring recurrent point mutations in the ubiquitin ligase adaptor protein SPOP and discuss opportunities for future clinical translation. More specifically, activation of the androgen receptor (AR) signaling emerges as the key oncogenic pathway. SPOP-mutant prostate cancer patients respond to AR inhibition in various clinical settings. Molecular insights on how mutant SPOP promotes tumorigenesis may open more specific therapeutic avenues which, in combination with conventional AR-targeting agents, could improve the outcome of patients with SPOP-mutant prostate cancer.
引用
收藏
页码:11 / 18
页数:8
相关论文
共 94 条
[1]   Genomic correlates of clinical outcome in advanced prostate cancer [J].
Abida, Wassim ;
Cyrta, Joanna ;
Heller, Glenn ;
Prandi, Davide ;
Armenia, Joshua ;
Coleman, Ilsa ;
Cieslik, Marcin ;
Benelli, Matteo ;
Robinson, Dan ;
Van Allen, Eliezer M. ;
Sboner, Andrea ;
Fedrizzi, Tarcisio ;
Mosquera, Juan Miguel ;
Robinson, Brian D. ;
De Sarkar, Navonil ;
Kunju, Lakshmi P. ;
Tomlins, Scott ;
Wu, Yi Mi ;
Rodrigues, Daniel Nava ;
Loda, Massimo ;
Gopalan, Anuradha ;
Reuter, Victor E. ;
Pritchard, Colin C. ;
Mateo, Joaquin ;
Bianchini, Diletta ;
Miranda, Susana ;
Carreira, Suzanne ;
Rescigno, Pasquale ;
Filipenko, Julie ;
Vinson, Jacob ;
Montgomery, Robert B. ;
Beltran, Himisha ;
Heath, Elisabeth I. ;
Scher, Howard I. ;
Kantoff, Philip W. ;
Taplin, Mary-Ellen ;
Schultz, Nikolaus ;
deBono, Johann S. ;
Demichelis, Francesca ;
Nelson, Peter S. ;
Rubin, Mark A. ;
Chinnaiyan, Arul M. ;
Sawyers, Charles L. .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 2019, 116 (23) :11428-11436
[2]   FOXA1 mutations alter pioneering activity, differentiation and prostate cancer phenotypes [J].
Adams, Elizabeth J. ;
Karthaus, Wouter R. ;
Hoover, Elizabeth ;
Liu, Deli ;
Gruet, Antoine ;
Zhang, Zeda ;
Cho, Hyunwoo ;
DiLoreto, Rose ;
Chhangawala, Sagar ;
Liu, Yang ;
Watson, Philip A. ;
Davicioni, Elai ;
Sboner, Andrea ;
Barbieri, Christopher E. ;
Bose, Rohit ;
Leslie, Christina S. ;
Sawyers, Charles L. .
NATURE, 2019, 571 (7765) :408-+
[3]   Trim24 targets endogenous p53 for degradation [J].
Allton, Kendra ;
Jain, Abhinav K. ;
Herz, Hans-Martin ;
Tsai, Wen-Wei ;
Jung, Sung Yun ;
Qin, Jun ;
Bergmann, Andreas ;
Johnson, Randy L. ;
Barton, Michelle Craig .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 2009, 106 (28) :11612-11616
[4]   Truncated ERG Oncoproteins from TMPRSS2-ERG Fusions Are Resistant to SPOP-Mediated Proteasome Degradation [J].
An, Jian ;
Ren, Shancheng ;
Murphy, Stephen J. ;
Dalangood, Sumiya ;
Chang, Cunjie ;
Pang, Xiaodong ;
Cui, Yangyan ;
Wang, Liguo ;
Pan, Yunqian ;
Zhang, Xiaowei ;
Zhu, Yasheng ;
Wang, Chenji ;
Halling, Geoffrey C. ;
Cheng, Liang ;
Sukov, William R. ;
Karnes, R. Jeffrey ;
Vasmatzis, George ;
Zhang, Qing ;
Zhang, Jun ;
Cheville, John C. ;
Yan, Jun ;
Sun, Yinghao ;
Huang, Haojie .
MOLECULAR CELL, 2015, 59 (06) :904-916
[5]   Destruction of Full-Length Androgen Receptor by Wild-Type SPOP, but Not Prostate-Cancer-Associated Mutants [J].
An, Jian ;
Wang, Chenji ;
Deng, Yibin ;
Yu, Long ;
Huang, Haojie .
CELL REPORTS, 2014, 6 (04) :657-669
[6]   Small-molecule PROTACs: An emerging and promising approach for the development of targeted therapy drugs [J].
An, Sainan ;
Fu, Liwu .
EBIOMEDICINE, 2018, 36 :553-562
[7]   Circulating Tumor DNA Genomics Correlate with Resistance to Abiraterone and Enzalutamide in Prostate Cancer [J].
Annala, Matti ;
Vandekerkhove, Gillian ;
Khalaf, Daniel ;
Taavitsainen, Sinja ;
Beja, Kevin ;
Warner, Evan W. ;
Sunderland, Katherine ;
Kollmannsberger, Christian ;
Eigl, Bernhard J. ;
Finch, Daygen ;
Oja, Conrad D. ;
Vergidis, Joanna ;
Zulfiqar, Muhammad ;
Azad, Arun A. ;
Nykter, Matti ;
Gleave, Martin E. ;
Wyatt, Alexander W. ;
Chi, Kim N. .
CANCER DISCOVERY, 2018, 8 (04) :444-457
[8]   The long tail of oncogenic drivers in prostate cancer [J].
Armenia, Joshua ;
Wankowicz, Stephanie A. M. ;
Liu, David ;
Gao, Jianjiong ;
Kundra, Ritika ;
Reznik, Ed ;
Chatila, Walid K. ;
Chakravarty, Debyani ;
Han, G. Celine ;
Coleman, Ilsa ;
Montgomery, Bruce ;
Pritchard, Colin ;
Morrissey, Colm ;
Barbieri, Christopher E. ;
Beltran, Himisha ;
Sboner, Andrea ;
Zafeiriou, Zafeiris ;
Miranda, Susana ;
Bielski, Craig M. ;
Penson, Alexander V. ;
Tolonen, Charlotte ;
Huang, Franklin W. ;
Robinson, Dan ;
Wu, Yi Mi ;
Lonigro, Robert ;
Garraway, Levi A. ;
Demichelis, Francesca ;
Kantoff, Philip W. ;
Taplin, Mary-Ellen ;
Abida, Wassim ;
Taylor, Barry S. ;
Scher, Howard I. ;
Nelson, Peter S. ;
de Bono, Johann S. ;
Rubin, Mark A. ;
Sawyers, Charles L. ;
Chinnaiyan, Arul M. ;
Schultz, Nikolaus ;
Van Allen, Eliezer M. .
NATURE GENETICS, 2018, 50 (05) :645-+
[9]   Therapeutic targeting of BET bromodomain proteins in castration-resistant prostate cancer [J].
Asangani, Irfan A. ;
Dommeti, Vijaya L. ;
Wang, Xiaoju ;
Malik, Rohit ;
Cieslik, Marcin ;
Yang, Rendong ;
Escara-Wilke, June ;
Wilder-Romans, Kari ;
Dhanireddy, Sudheer ;
Engelke, Carl ;
Iyer, Mathew K. ;
Jing, Xiaojun ;
Wu, Yi-Mi ;
Cao, Xuhong ;
Qin, Zhaohui S. ;
Wang, Shaomeng ;
Feng, Felix Y. ;
Chinnaiyan, Arul M. .
NATURE, 2014, 510 (7504) :278-+
[10]  
Augello M.A., 2019, CANCER CELL, V35, pe608
12345678910