Discovery and Pharmacological Characterization of JNJ-42756493 (Erdafitinib), a Functionally Selective Small-Molecule FGFR Family Inhibitor

Overview

Journal Mol Cancer Ther

Date 2017 Mar 26

PMID 28341788

Citations 132

Authors

Timothy P S Perera

Eleonora Jovcheva

Laurence Mevellec

Jorge Vialard

Desiree De Lange

Tinne Verhulst

Caroline Paulussen

Kelly van de Ven

Peter King

Eddy Freyne

David C Rees

Matthew Squires

Gordon Saxty

Martin Page

Christopher W Murray

Ron Gilissen

George Ward

Neil T Thompson

David R Newell

Na Cheng

Liang Xie

Jennifer Yang

Suso J Platero

Jayaprakash D Karkera

Christopher Moy

Patrick Angibaud

Sylvie Laquerre

Matthew V Lorenzi

Affiliations

Soon will be listed here.

Abstract

Fibroblast growth factor (FGF) signaling plays critical roles in key biological processes ranging from embryogenesis to wound healing and has strong links to several hallmarks of cancer. Genetic alterations in FGF receptor () family members are associated with increased tumor growth, metastasis, angiogenesis, and decreased survival. JNJ-42756493, erdafitinib, is an orally active small molecule with potent tyrosine kinase inhibitory activity against all four FGFR family members and selectivity versus other highly related kinases. JNJ-42756493 shows rapid uptake into the lysosomal compartment of cells in culture, which is associated with prolonged inhibition of FGFR signaling, possibly due to sustained release of the inhibitor. In xenografts from human tumor cell lines or patient-derived tumor tissue with activating FGFR alterations, JNJ-42756493 administration results in potent and dose-dependent antitumor activity accompanied by pharmacodynamic modulation of phospho-FGFR and phospho-ERK in tumors. The results of the current study provide a strong rationale for the clinical investigation of JNJ-42756493 in patients with tumors harboring FGFR pathway alterations. .

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