TY - JOUR
T1 - Reducing MYC's transcriptional footprint unveils a good prognostic gene signature in melanoma
AU - Zacarías-Fluck, Mariano F
AU - Massó Vallés, Daniel
AU - Giuntini, Fabio
AU - González-Larreategui, Íñigo
AU - Kaur, Jastrinjan
AU - Casacuberta-Serra, Sílvia
AU - Jauset, Toni
AU - Martínez-Martín, Sandra
AU - Martín-Fernández, Génesis
AU - Serrano del Pozo, Erika
AU - Foradada, Laia
AU - Grueso, Judit
AU - Nonell, Lara
AU - Beaulieu, Marie-Eve
AU - Whitfield, Jonathan R.
AU - Soucek, Laura
N1 - Publisher Copyright:
© 2023 Zacarías-Fluck et al.
PY - 2023/4/6
Y1 - 2023/4/6
N2 - MYC's key role in oncogenesis and tumor progression has long been established for most human cancers. In melanoma, its deregulated activity by amplification of 8q24 chromosome or by upstream signaling coming from activating mutations in the RAS/RAF/MAPK pathway-the most predominantly mutated pathway in this disease-turns MYC into not only a driver but also a facilitator of melanoma progression, with documented effects leading to an aggressive clinical course and resistance to targeted therapy. Here, by making use of Omomyc, the most characterized MYC inhibitor to date that has just successfully completed a phase I clinical trial, we show for the first time that MYC inhibition in melanoma induces remarkable transcriptional modulation, resulting in severely compromised tumor growth and a clear abrogation of metastatic capacity independently of the driver mutation. By reducing MYC's transcriptional footprint in melanoma, Omomyc elicits gene expression profiles remarkably similar to those of patients with good prognosis, underlining the therapeutic potential that such an approach could eventually have in the clinic in this dismal disease.
AB - MYC's key role in oncogenesis and tumor progression has long been established for most human cancers. In melanoma, its deregulated activity by amplification of 8q24 chromosome or by upstream signaling coming from activating mutations in the RAS/RAF/MAPK pathway-the most predominantly mutated pathway in this disease-turns MYC into not only a driver but also a facilitator of melanoma progression, with documented effects leading to an aggressive clinical course and resistance to targeted therapy. Here, by making use of Omomyc, the most characterized MYC inhibitor to date that has just successfully completed a phase I clinical trial, we show for the first time that MYC inhibition in melanoma induces remarkable transcriptional modulation, resulting in severely compromised tumor growth and a clear abrogation of metastatic capacity independently of the driver mutation. By reducing MYC's transcriptional footprint in melanoma, Omomyc elicits gene expression profiles remarkably similar to those of patients with good prognosis, underlining the therapeutic potential that such an approach could eventually have in the clinic in this dismal disease.
KW - MYC
KW - Omomyc
KW - melanoma
KW - signature
UR - http://www.scopus.com/inward/record.url?scp=85153804594&partnerID=8YFLogxK
UR - https://www.mendeley.com/catalogue/3c137d5a-6016-30f1-ac4e-f0fe0e58c941/
U2 - 10.1101/gad.350078.122
DO - 10.1101/gad.350078.122
M3 - Article
C2 - 37024284
SN - 0890-9369
VL - 37
SP - 303
EP - 320
JO - Genes and Development
JF - Genes and Development
ER -