Massive parallel sequencing uncovers actionable FGFR2–PPHLN1 fusion and ARAF mutations in intrahepatic cholangiocarcinoma

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作者
Daniela Sia
Bojan Losic
Agrin Moeini
Laia Cabellos
Ke Hao
Kate Revill
Dennis Bonal
Oriana Miltiadous
Zhongyang Zhang
Yujin Hoshida
Helena Cornella
Mireia Castillo-Martin
Roser Pinyol
Yumi Kasai
Sasan Roayaie
Swan N. Thung
Josep Fuster
Myron E. Schwartz
Samuel Waxman
Carlos Cordon-Cardo
Eric Schadt
Vincenzo Mazzaferro
Josep M. Llovet
机构
[1] Barcelona-Clínic Liver Cancer Group (HCC Translational Research Laboratory,Department of Surgery
[2] Liver Unit,Mount Sinai Liver Cancer Program (Divisions of Liver Diseases, Department of Medicine, Department of Pathology
[3] Hepato-biliary Surgery),undefined
[4] Institut d’Investigacions Biomèdiques August Pi i Sunyer (IDIBAPS),undefined
[5] Hospital Clínic,undefined
[6] CIBERehd,undefined
[7] Universitat de Barcelona,undefined
[8] Gastrointestinal Surgery and Liver Transplantation Unit,undefined
[9] National Cancer Institute,undefined
[10] Recanati Miller Transplantation Institute),undefined
[11] Tisch Cancer Institute,undefined
[12] Icahn School of Medicine at Mount Sinai,undefined
[13] Icahn Institute for Genomics and Multiscale Biology,undefined
[14] Icahn School of Medicine at Mount Sinai,undefined
[15] Liver Cancer Program,undefined
[16] Hofstra-North Shore LIJ School of Medicine,undefined
[17] Lenox Hill Hospital,undefined
[18] Institució Catalana de Recerca i Estudis Avançats,undefined
来源
Nature Communications | / 6卷
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摘要
Intrahepatic cholangiocarcinoma (iCCA) is a fatal bile duct cancer with dismal prognosis and limited therapeutic options. By performing RNA- and exome-sequencing analyses, we report a novel fusion event, FGFR2–PPHLN1 (16%), and damaging mutations in the ARAF oncogene (11%). Here we demonstrate that the chromosomal translocation t(10;12)(q26;q12) leading to FGFR2–PPHLN1 fusion possesses transforming and oncogenic activity, which is successfully inhibited by a selective FGFR2 inhibitor in vitro. Among the ARAF mutations, N217I and G322S lead to activation of the pathway and N217I shows oncogenic potential in vitro. Screening of a cohort of 107 iCCA patients reveals that FGFR2 fusions represent the most recurrent targetable alteration (45%, 17/107), while they are rarely present in other primary liver tumours (0/100 of hepatocellular carcinoma (HCC); 1/21 of mixed iCCA-HCC). Taken together, around 70% of iCCA patients harbour at least one actionable molecular alteration (FGFR2 fusions, IDH1/2, ARAF, KRAS, BRAF and FGF19) that is amenable for therapeutic targeting.
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