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Por favor, use este identificador para citar o enlazar este ítem: http://documenta.ciemat.es/handle/123456789/2301

Título : Intrinsic cell-penetrating activity propels Omomyc from proof of concept to viable anti-Myc therapy
Autor : Beaulieu, Marie-Eve
Jauset, Toni
Massó-Vallés, Daniel
Martínez-Martín, Sandra
Rahl, Peter
Maltais, Loïka
Zacarias-Fluck, Mariano F.
Casacuberta-Serra, Silvia
Serrano del Pozo, Erika
Fiore, Christopher
Foradada, Laia
Castillo Cano, Virginia
Sánchez-Hervás, Maritxel
Guenther, Matthew
Romero Sanz, Eduardo
Oteo, Marta
Temblay, Cynthia
Martin, Génesis
Letourneau, Danny
Montagne, Martin
Morcillo Alonso, Miguel Ángel
Whitfield, Jonathan R.
Lavigne, Pierre
Soucek, Laura
Fecha de publicación : 1-feb-2024
Resumen : Inhibiting MYC has long been considered unfeasible, although its key role in human cancers makes it a desirable target for therapeutic intervention. One reason for its perceived undruggability was the fear of catastrophic side effects in normal tissues. However, we previously designed a dominant-negative form of MYC called Omomyc and used its conditional transgenic expression to inhibit MYC function both in vitro and in vivo. MYC inhibition by Omomyc exerted a potent therapeutic impact in various mouse models of cancer, causing only mild, well-tolerated, and reversible side effects. Nevertheless, Omomyc has been so far considered only a proof of principle. In contrast with that preconceived notion, here, we show that the purified Omomyc mini-protein itself spontaneously penetrates into cancer cells and effectively interferes with MYC transcriptional activity therein. Efficacy of the Omomyc mini-protein in various experimental models of non-small cell lung cancer harboring different oncogenic mutation profiles establishes its therapeutic potential after both direct tissue delivery and systemic administration, providing evidence that the Omomyc mini-protein is an effective MYC inhibitor worthy of clinical development.
URI : http://documenta.ciemat.es/handle/123456789/2301
ISSN : 1946-6234
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