Resistance to Selective FGFR Inhibitors in FGFR- Driven Urothelial Cancer

被引:39
作者
Facchinetti, Francesco [1 ]
Hollebecque, Antoine [2 ,3 ]
Braye, Floriane [1 ]
Vasseur, Damien [4 ,5 ]
Pradat, Yoann [6 ]
Bahleda, Rastislav [2 ]
Pobel, Cedric [1 ]
Bigot, Ludovic [1 ]
Deas, Olivier [7 ]
Arango, Juan DavidFlorez [1 ]
Guaitoli, Giorgia [1 ,8 ]
Mizuta, Hayato [1 ]
Combarel, David [4 ]
Tselikas, Lambros [9 ]
Michiels, Stefan [10 ,11 ]
Nikolaev, Sergey I. [1 ]
Scoazec, Jean-Yves [4 ,5 ,12 ]
Ponce-Aix, Santiago [1 ,2 ]
Besse, Benjamin [1 ,3 ,12 ]
Olaussen, Ken A. [1 ,12 ]
Loriot, Yohann [1 ,2 ,3 ]
Friboulet, Luc [1 ,13 ]
机构
[1] Univ Paris Saclay, Gustave Roussy, INSERM, U981, Villejuif, France
[2] Gustave Roussy, Dept Innovat Therapeut DITEP, Villejuif, France
[3] Gustave Roussy, Dept Medecine Oncol, Villejuif, France
[4] Gustave Roussy, Med Biol & Pathol Dept, Villejuif, France
[5] Gustave Roussy, AMMICa UAR3655 US23, Villejuif, France
[6] Univ Paris Saclay, MICS Lab, Cent Supelec, Lab EM2C, Gif Sur Yvette, France
[7] XenTech, Evry, France
[8] Univ Modena & Reggio Emilia, PhD Program Clin & Expt Med, Modena, Italy
[9] Univ Paris Saclay, Dept Intervent Radiol, BIOTHERIS, Gustave Roussy, Villejuif, France
[10] Univ Paris Saclay, INSERM, CESP, Villejuif, France
[11] Gustave Roussy, Off Biostat & Epidemiol, Villejuif, France
[12] Univ Paris Saclay, Fac Med, Le Kremlin Bicetre, France
[13] Gustave Roussy Canc Campus, INSERM, U981, 114 Rue Edouard Vaillant, F-94800 Villejuif, France
来源
CANCER DISCOVERY | 2023年 / 13卷 / 09期
关键词
ACQUIRED-RESISTANCE; EGFR; MUTATIONS; ACTIVATION; EVEROLIMUS; MECHANISM;
D O I
10.1158/2159-8290.CD-22-1441
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Several fibroblast growth factor receptor (FGFR) inhibitors are approved or in clinical development for the treatment of FGFR-driven urothelial cancer, and molecular mechanisms of resistance leading to patient relapses have not been fully explored. We identified 21 patients with FGFR-driven urothelial cancer treated with selective FGFR inhibitors and analyzed postprogression tissue and/or circulating tumor DNA (ctDNA). We detected single mutations in the FGFR tyrosine kinase domain in seven (33%) patients (FGFR3 N540K, V553L/M, V555L/M, E587Q; FGFR2 L551F) and multiple mutations in one (5%) case (FGFR3 N540K, V555L, and L608V). Using Ba/F3 cells, we defined their spectrum of resistance/sensitivity to multiple selective FGFR inhibitors. Eleven (52%) patients harbored alterations in the PI3K-mTOR pathway ( n = 4 TSC1/2, n = 4 PIK3CA, n = 1 TSC1 and PIK3CA, n = 1 NF2, n = 1 PTEN). In patient derived models, erdafitinib was synergistic with pictilisib in the presence of PIK3CA E545K, whereas erdafitinib-gefitinib combination was able to overcome bypass resistance mediated by EGFR activation. SIGNIFICANCE: In the largest study on the topic thus far, we detected a high frequency of FGFR kinase domain mutations responsible for resistance to FGFR inhibitors in urothelial cancer. Off-target resistance mechanisms involved primarily the PI3K-mTOR pathway. Our findings provide preclinical evidence sustaining combinatorial treatment strategies to overcome bypass resistance. See related commentary by Tripathi et al., p. 1964.
引用
收藏
页码:1998 / 2011
页数:14
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