FB2024_03 , released June 25, 2024
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Citation
Frattini, V., Pagnotta, S.M., Tala, , Fan, J.J., Russo, M.V., Lee, S.B., Garofano, L., Zhang, J., Shi, P., Lewis, G., Sanson, H., Frederick, V., Castano, A.M., Cerulo, L., Rolland, D.C.M., Mall, R., Mokhtari, K., Elenitoba-Johnson, K.S.J., Sanson, M., Huang, X., Ceccarelli, M., Lasorella, A., Iavarone, A. (2018). A metabolic function of FGFR3-TACC3 gene fusions in cancer.  Nature 553(7687): 222--227.
FlyBase ID
FBrf0241601
Publication Type
Research paper
Abstract
Chromosomal translocations that generate in-frame oncogenic gene fusions are notable examples of the success of targeted cancer therapies. We have previously described gene fusions of FGFR3-TACC3 (F3-T3) in 3% of human glioblastoma cases. Subsequent studies have reported similar frequencies of F3-T3 in many other cancers, indicating that F3-T3 is a commonly occuring fusion across all tumour types. F3-T3 fusions are potent oncogenes that confer sensitivity to FGFR inhibitors, but the downstream oncogenic signalling pathways remain unknown. Here we show that human tumours with F3-T3 fusions cluster within transcriptional subgroups that are characterized by the activation of mitochondrial functions. F3-T3 activates oxidative phosphorylation and mitochondrial biogenesis and induces sensitivity to inhibitors of oxidative metabolism. Phosphorylation of the phosphopeptide PIN4 is an intermediate step in the signalling pathway of the activation of mitochondrial metabolism. The F3-T3-PIN4 axis triggers the biogenesis of peroxisomes and the synthesis of new proteins. The anabolic response converges on the PGC1α coactivator through the production of intracellular reactive oxygen species, which enables mitochondrial respiration and tumour growth. These data illustrate the oncogenic circuit engaged by F3-T3 and show that F3-T3-positive tumours rely on mitochondrial respiration, highlighting this pathway as a therapeutic opportunity for the treatment of tumours with F3-T3 fusions. We also provide insights into the genetic alterations that initiate the chain of metabolic responses that drive mitochondrial metabolism in cancer.
PubMed ID
29323298
PubMed Central ID
PMC5771419 (PMC) (EuropePMC)
DOI
10.1038/nature25171
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Secondary IDs
    Language of Publication
    English
    Additional Languages of Abstract
    Parent Publication
    Publication Type
    Journal
    Abbreviation
    Nature
    Title
    Nature
    Publication Year
    1869-
    ISBN/ISSN
    0028-0836
    Data From Reference