FGF19 and its analog Aldafermin cooperate with MYC to induce aggressive hepatocarcinogenesis - Institut de génétique moléculaire de Montpellier Accéder directement au contenu
Article Dans Une Revue EMBO Molecular Medicine Année : 2024

FGF19 and its analog Aldafermin cooperate with MYC to induce aggressive hepatocarcinogenesis

José Ursic-Bedoya
Guillaume Desandré
  • Fonction : co premier-auteur
  • PersonId : 1124015
Arnaud Polizzi
Benjamin Rivière
  • Fonction : Auteur
Hervé Guillou
Eric Assenat
  • Fonction : Auteur

Résumé

FGF19 hormone has pleiotropic metabolic functions, including the modulation of insulin sensitivity, glucose/lipid metabolism and energy homeostasis. On top of its physiological metabolic role, FGF19 has been identified as a potentially targetable oncogenic driver, notably in hepatocellular carcinoma (HCC). Nevertheless, FGF19 remained an attractive candidate for treatment of metabolic disease, prompting the development of analogs uncoupling its metabolic and tumor-promoting activities. Using pre-clinical mice models of somatic mutation driven HCC, we assessed the oncogenicity of FGF19 in combination with frequent HCC tumorigenic alterations: p53 inactivation, CTNNB1 mutation, CCND1 or MYC overexpression. Our data revealed a strong oncogenic cooperation between FGF19 and MYC. Most importantly, we show that this oncogenic synergy is conserved with a FGF19-analog Aldafermin (NGM282), designed to solely mimic the hormone's metabolic functions. In particular, even a short systemic treatment with recombinant proteins triggered rapid appearance of proliferative foci of MYC-expressing hepatocytes. The fact that FGF19 analog Aldafermin is not fully devoid of the hormone's oncogenic properties raises concerns in the context of its potential use for patients with damaged, mutation-prone liver.
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Dates et versions

hal-04404913 , version 1 (19-01-2024)

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Citer

José Ursic-Bedoya, Guillaume Desandré, Carine Chavey, Pauline Marie, Arnaud Polizzi, et al.. FGF19 and its analog Aldafermin cooperate with MYC to induce aggressive hepatocarcinogenesis. EMBO Molecular Medicine, 2024, ⟨10.1038/s44321-023-00021-x⟩. ⟨hal-04404913⟩
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