UMYMFOR   05516
UNIDAD DE MICROANALISIS Y METODOS FISICOS EN QUIMICA ORGANICA
Unidad Ejecutora - UE
artículos
Título:
New inhibitor targeting Acyl-CoA synthetase 4 reduces breast and prostate tumor growth, therapeutic resistance and steroidogenesis
Autor/es:
CASTILLO, ANA F.; PRADA, JESICA G.; BIGI, MARÍA M.; INDO, SEBASTIÁN; MARELLI, BELKIS E.; ORTEGA, HUGO H.; GOMEZ, DANIEL E.; ORLANDO, ULISES D.; DATTILO, MELINA A.; RÍOS MEDRANO, MAYRA A.; CAROCA, GRACIELA; SALINAS, FACUNDO J.; LORENZANO MENNA, PABLO; RODRÍGUEZ, JUAN B.; MALOBERTI, PAULA M.; SOLANO, ANGELA R.; TORRES, MARÍA T.; CONTRERAS, HECTOR R.; SALVETTI, NATALIA R.; SZAJNMAN, SERGIO; PODESTA, ERNESTO J.
Revista:
CELL. MOLEC. LIFE SCIEN.
Editorial:
Springer Science and Business Media Deutschland GmbH
Referencias:
Año: 2021 vol. 78 p. 2893 - 2910
ISSN:
1420-682X
Resumen:
Acyl-CoA synthetase 4 (ACSL4) is an isoenzyme of the fatty acid ligase-coenzyme-A family taking part in arachidonic acid metabolism and steroidogenesis. ACSL4 is involved in the development of tumor aggressiveness in breast and prostate tumors through the regulation of various signal transduction pathways. Here, a bioinformatics analysis shows that the ACSL4 gene expression and proteomic signatures obtained using a cell model was also observed in tumor samples from breast and cancer patients. A well-validated ACSL4 inhibitor, however, has not been reported hindering the full exploration of this promising target and its therapeutic application on cancer and steroidogenesis inhibition. In this study, ACSL4 inhibitor PRGL493 was identified using a homology model for ACSL4 and docking based virtual screening. PRGL493 was then chemically characterized through nuclear magnetic resonance and mass spectroscopy. The inhibitory activity was demonstrated through the inhibition of arachidonic acid transformation into arachidonoyl-CoA using the recombinant enzyme and cellular models. The compound blocked cell proliferation and tumor growth in both breast and prostate cellular and animal models and sensitized tumor cells to chemotherapeutic and hormonal treatment. Moreover, PGRL493 inhibited de novo steroid synthesis in testis and adrenal cells, in a mouse model and in prostate tumor cells. This work provides proof of concept for the potential application of PGRL493 in clinical practice. Also, these findings may prove key to therapies aiming at the control of tumor growth and drug resistance in tumors which express ACSL4 and depend on steroid synthesis.