Gene expression profiling of patient-derived pancreatic cancer xenografts predicts sensitivity to the BET bromodomain inhibitor JQ1: implications for individualized medicine efforts

被引:57
作者
Bian, Benjamin [1 ,2 ]
Bigonnet, Martin [1 ,2 ]
Gayet, Odile [1 ,2 ]
Loncle, Celine [1 ,2 ]
Maignan, Aurelie [1 ,2 ]
Gilabert, Marine [1 ,2 ]
Moutardier, Vincent [1 ,2 ,3 ,4 ]
Garcia, Stephane [1 ,2 ,3 ]
Turrini, Olivier [1 ,2 ,5 ]
Delpero, Jean-Robert [5 ]
Giovannini, Marc [5 ]
Grandval, Philippe [6 ]
Gasmi, Mohamed [3 ,4 ]
Ouaissi, Mehdi [6 ]
Secq, Veronique [3 ]
Poizat, Flora [5 ]
Nicolle, Remy [7 ]
Blum, Yuna [7 ]
Marisa, Laetitia [7 ]
Rubis, Marion [1 ,2 ]
Raoul, Jean-Luc [5 ]
Bradner, James E. [8 ]
Qi, Jun [8 ]
Lomberk, Gwen [9 ,10 ]
Urrutia, Raul [9 ,10 ]
Saul, Andres [11 ]
Dusetti, Nelson [1 ,2 ]
Iovanna, Juan [1 ,2 ]
机构
[1] Aix Marseille Univ, CNRS UMR 7258, INSERM U1068, CRCM, Parc Sci & Technol Luminy, Marseille, France
[2] Inst Paoli Calmettes, Marseille, France
[3] Hop Nord Marseille, Marseille, France
[4] Aix Marseille Univ, Hop Nord, AP HM, CIC1409, Marseille, France
[5] Inst Paoli Calmettes, Marseille, France
[6] Hop La Timone, Marseille, France
[7] Ligue Natl Canc, Programme Cartes Identite Tumeurs CIT, Paris, France
[8] Harvard Med Sch, Dana Farber Canc Inst, Dept Med Oncol, Boston, MA USA
[9] Mayo Clin, Dept Biochem & Mol Biol, Lab Epigenet & Chromatin Dynam, Rochester, MN USA
[10] Mayo Clin, Dept Med, Lab Epigenet & Chromatin Dynam, Rochester, MN USA
[11] Aix Marseille Univ, CNRS UMR 7325, Ctr Interdisciplinaire Nanosci Marseille, Parc Sci & Technol Luminy, Marseille, France
关键词
bromodomains; c-MYC; JQ1; pancreatic adenocarcinoma; transcriptomic signature; C-MYC; THERAPY; GROWTH; STRATIFICATION; TRANSCRIPTION; ACTIVATION; PROTEINS; NORMALIZATION; GEMCITABINE; MECHANISMS;
D O I
10.15252/emmm.201606975
中图分类号
R-3 [医学研究方法]; R3 [基础医学];
学科分类号
1001 ;
摘要
c-MYC controls more than 15% of genes responsible for proliferation, differentiation, and cellular metabolism in pancreatic as well as other cancers making this transcription factor a prime target for treating patients. The transcriptome of 55 patient-derived xenografts show that 30% of them share an exacerbated expression profile of MYC transcriptional targets (MYC-high). This cohort is characterized by a high level of Ki67 staining, a lower differentiation state, and a shorter survival time compared to the MYC-low subgroup. To define classifier expression signature, we selected a group of 10 MYC target transcripts which expression is increased in the MYC-high group and six transcripts increased in the MYClow group. We validated the ability of these markers panel to identify MYC-high patient-derived xenografts from both: discovery and validation cohorts as well as primary cell cultures from the same patients. We then showed that cells from MYC-high patients are more sensitive to JQ1 treatment compared to MYC-low cells, in monolayer, 3D cultured spheroids and in vivo xenografted tumors, due to cell cycle arrest followed by apoptosis. Therefore, these results provide new markers and potentially novel therapeutic modalities for distinct subgroups of pancreatic tumors and may find application to the future management of these patients within the setting of individualized medicine clinics.
引用
收藏
页码:482 / 497
页数:16
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