Truncated FGFR2 is a clinically actionable oncogene in multiple cancers.

Zingg, Daniel; Bhin, Jinhyuk; Yemelyanenko, Julia; Kas, Sjors M; Rolfs, Frank; Lutz, Catrin; Lee, Jessica K; Klarenbeek, Sjoerd; Silverman, Ian M; Annunziato, Stefano; Chan, Chang S; Piersma, Sander R; Eijkman, Timo; Badoux, Madelon; Gogola, Ewa; Siteur, Bjørn; Sprengers, Justin; de Klein, Bim; de Goeij-de Haas, Richard R; Riedlinger, Gregory M; Ke, Hua; Madison, Russell; Drenth, Anne Paulien; van der Burg, Eline; Schut, Eva; Henneman, Linda; van Miltenburg, Martine H; Proost, Natalie; Zhen, Huiling; Wientjens, Ellen; de Bruijn, Roebi; de Ruiter, Julian R; Boon, Ute; de Korte-Grimmerink, Renske; van Gerwen, Bastiaan; Féliz, Luis; Abou-Alfa, Ghassan K; Ross, Jeffrey S; van de Ven, Marieke; Rottenberg, Sven; Cuppen, Edwin; Chessex, Anne Vaslin; Ali, Siraj M; Burn, Timothy C; Jimenez, Connie R; Ganesan, Shridar; Wessels, Lodewyk F A; Jonkers, Jos

doi:10.48350/171911

Publication:
Truncated FGFR2 is a clinically actionable oncogene in multiple cancers.

cris.virtual.author-orcid	0000-0003-2044-9844
cris.virtualsource.author-orcid	3ce5c712-81bb-4245-9893-0aa479809c45
datacite.rights	open.access
dc.contributor.author	Zingg, Daniel
dc.contributor.author	Bhin, Jinhyuk
dc.contributor.author	Yemelyanenko, Julia
dc.contributor.author	Kas, Sjors M
dc.contributor.author	Rolfs, Frank
dc.contributor.author	Lutz, Catrin
dc.contributor.author	Lee, Jessica K
dc.contributor.author	Klarenbeek, Sjoerd
dc.contributor.author	Silverman, Ian M
dc.contributor.author	Annunziato, Stefano
dc.contributor.author	Chan, Chang S
dc.contributor.author	Piersma, Sander R
dc.contributor.author	Eijkman, Timo
dc.contributor.author	Badoux, Madelon
dc.contributor.author	Gogola, Ewa
dc.contributor.author	Siteur, Bjørn
dc.contributor.author	Sprengers, Justin
dc.contributor.author	de Klein, Bim
dc.contributor.author	de Goeij-de Haas, Richard R
dc.contributor.author	Riedlinger, Gregory M
dc.contributor.author	Ke, Hua
dc.contributor.author	Madison, Russell
dc.contributor.author	Drenth, Anne Paulien
dc.contributor.author	van der Burg, Eline
dc.contributor.author	Schut, Eva
dc.contributor.author	Henneman, Linda
dc.contributor.author	van Miltenburg, Martine H
dc.contributor.author	Proost, Natalie
dc.contributor.author	Zhen, Huiling
dc.contributor.author	Wientjens, Ellen
dc.contributor.author	de Bruijn, Roebi
dc.contributor.author	de Ruiter, Julian R
dc.contributor.author	Boon, Ute
dc.contributor.author	de Korte-Grimmerink, Renske
dc.contributor.author	van Gerwen, Bastiaan
dc.contributor.author	Féliz, Luis
dc.contributor.author	Abou-Alfa, Ghassan K
dc.contributor.author	Ross, Jeffrey S
dc.contributor.author	van de Ven, Marieke
dc.contributor.author	Rottenberg, Sven
dc.contributor.author	Cuppen, Edwin
dc.contributor.author	Chessex, Anne Vaslin
dc.contributor.author	Ali, Siraj M
dc.contributor.author	Burn, Timothy C
dc.contributor.author	Jimenez, Connie R
dc.contributor.author	Ganesan, Shridar
dc.contributor.author	Wessels, Lodewyk F A
dc.contributor.author	Jonkers, Jos
dc.date.accessioned	2024-10-11T17:00:14Z
dc.date.available	2024-10-11T17:00:14Z
dc.date.issued	2022-08
dc.description.abstract	Somatic hotspot mutations and structural amplifications and fusions that affect fibroblast growth factor receptor 2 (encoded by FGFR2) occur in multiple types of cancer1. However, clinical responses to FGFR inhibitors have remained variable1-9, emphasizing the need to better understand which FGFR2 alterations are oncogenic and therapeutically targetable. Here we apply transposon-based screening10,11 and tumour modelling in mice12,13, and find that the truncation of exon 18 (E18) of Fgfr2 is a potent driver mutation. Human oncogenomic datasets revealed a diverse set of FGFR2 alterations, including rearrangements, E1-E17 partial amplifications, and E18 nonsense and frameshift mutations, each causing the transcription of E18-truncated FGFR2 (FGFR2ΔE18). Functional in vitro and in vivo examination of a compendium of FGFR2ΔE18 and full-length variants pinpointed FGFR2-E18 truncation as single-driver alteration in cancer. By contrast, the oncogenic competence of FGFR2 full-length amplifications depended on a distinct landscape of cooperating driver genes. This suggests that genomic alterations that generate stable FGFR2ΔE18 variants are actionable therapeutic targets, which we confirmed in preclinical mouse and human tumour models, and in a clinical trial. We propose that cancers containing any FGFR2 variant with a truncated E18 should be considered for FGFR-targeted therapies.
dc.description.numberOfPages	9
dc.description.sponsorship	Department for BioMedical Research (DBMR)
dc.identifier.doi	10.48350/171911
dc.identifier.pmid	35948633
dc.identifier.publisherDOI	10.1038/s41586-022-05066-5
dc.identifier.uri	https://boris-portal.unibe.ch/handle/20.500.12422/86647
dc.language.iso	en
dc.publisher	Springer Nature
dc.relation.ispartof	Nature
dc.relation.issn	1476-4687
dc.relation.organization	DCD5A442C072E17DE0405C82790C4DE2
dc.relation.organization	DCD5A442BD18E17DE0405C82790C4DE2
dc.relation.url	https://boris.unibe.ch/172656/
dc.subject.ddc	600 - Technology::610 - Medicine & health
dc.subject.ddc	600 - Technology::630 - Agriculture
dc.title	Truncated FGFR2 is a clinically actionable oncogene in multiple cancers.
dc.type	article
dspace.entity.type	Publication
dspace.file.type	text
oaire.citation.endPage	617
oaire.citation.issue	7923
oaire.citation.startPage	609
oaire.citation.volume	608
oairecerif.author.affiliation	Department for BioMedical Research (DBMR)
oairecerif.author.affiliation2	Institut für Tierpathologie (ITPA)
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unibe.date.licenseChanged	2022-09-05 11:15:06
unibe.description.ispublished	pub
unibe.eprints.legacyId	171911
unibe.refereed	true
unibe.subtype.article	journal

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Truncated FGFR2 is a clinically actionable oncogene in multiple cancers.