Resistance to Selective FGFR Inhibitors in <i>FGFR-</i>Driven Urothelial Cancer-Reference-Cited by-同舟云学术

Resistance to Selective FGFR Inhibitors in FGFR-Driven Urothelial Cancer

Published:2023-06-28 Issue:9 Volume:13 Page:1998-2011
ISSN:2159-8274
Container-title:Cancer Discovery
language:en
Short-container-title:

Author:

Facchinetti Francesco¹^ORCID,Hollebecque Antoine²³^ORCID,Braye Floriane¹^ORCID,Vasseur Damien⁴⁵^ORCID,Pradat Yoann⁶^ORCID,Bahleda Rastislav²^ORCID,Pobel Cédric¹^ORCID,Bigot Ludovic¹^ORCID,Déas Olivier⁷^ORCID,Florez Arango Juan David¹^ORCID,Guaitoli Giorgia¹⁸^ORCID,Mizuta Hayato¹^ORCID,Combarel David⁴^ORCID,Tselikas Lambros⁹^ORCID,Michiels Stefan¹⁰¹¹^ORCID,Nikolaev Sergey I.¹^ORCID,Scoazec Jean-Yves⁴⁵¹²^ORCID,Ponce-Aix Santiago¹²^ORCID,Besse Benjamin¹³¹²^ORCID,Olaussen Ken A.¹¹²^ORCID,Loriot Yohann¹²³^ORCID,Friboulet Luc¹^ORCID

Affiliation:

1. 1Université Paris-Saclay, Gustave Roussy, Inserm U981, Villejuif, France.

2. 2Département d'Innovation Thérapeutique (DITEP), Gustave Roussy, Villejuif, France.

3. 3Département de Médecine Oncologique, Gustave Roussy, Villejuif, France.

4. 4Medical Biology and Pathology Department, Gustave Roussy, Villejuif, France.

5. 5AMMICa UAR3655/US23, Gustave Roussy, Villejuif, France.

6. 6Université Paris-Saclay, CentraleSupélec, MICS Lab, Gif-Sur-Yvette, France.

7. 7XenTech, Evry, France.

8. 8PhD Program Clinical and Experimental Medicine, University of Modena and Reggio Emilia, Modena, Italy.

9. 9BIOTHERIS, Department of Interventional Radiology, Gustave Roussy, Université Paris-Saclay, Villejuif, France.

10. 10Université Paris-Saclay, Inserm, CESP, Villejuif, France.

11. 11Gustave Roussy, Office of Biostatistics and Epidemiology, Villejuif, France.

12. 12Université Paris-Saclay, Faculté de Médecine, Le Kremlin Bicêtre, France.

Abstract

Abstract 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. This article is featured in Selected Articles from This Issue, p. 1949

Funder

European Research Council

Fondation Philanthropia

Fondation ARC pour la Recherche sur le Cancer

Fondation Gustave Roussy

Swiss Cancer Research Foundation

Publisher

American Association for Cancer Research (AACR)

Subject

Oncology

Link

https://aacrjournals.org/cancerdiscovery/article-pdf/doi/10.1158/2159-8290.CD-22-1441/3345110/cd-22-1441.pdf