FR58P1a; a new uncoupler of OXPHOS that inhibits migration in triple-negative breast cancer cells via Sirt1/AMPK/β1-integrin pathway

Urra, Félix A.; Hernández Muñoz, Felipe Andrés; Córdova Delgado, Miguel; Ramírez, María Paz; Peña Ahumada, Bárbara; Rios, Melany; Cruz, Pablo; Ahumada-Castro, Ulises; Bustos, Galdo; Silva-Pavez, Eduardo; Pulgar Tejo, Rodrigo; Morales, Danna; Varela, Diego; Millas-Vargas, Juan Pablo; Retamal

Artículos de revistas

Fecha

2018

Registro en:

Scientific Reports, Volumen 8, Issue 1, 2018,

20452322

10.1038/s41598-018-31367-9

https://repositorio.uchile.cl/handle/2250/167656

Autor

Urra, Félix A.

Hernández Muñoz, Felipe Andrés

Córdova Delgado, Miguel

Ramírez, María Paz

Peña Ahumada, Bárbara

Rios, Melany

Cruz, Pablo

Ahumada-Castro, Ulises

Bustos, Galdo

Silva-Pavez, Eduardo

Pulgar Tejo, Rodrigo

Morales, Danna

Varela, Diego

Millas-Vargas, Juan Pablo

Retamal

Institución

Universidad de Chile

Resumen

© 2018, The Author(s).Highly malignant triple-negative breast cancer (TNBC) cells rely mostly on glycolysis to maintain cellular homeostasis; however, mitochondria are still required for migration and metastasis. Taking advantage of the metabolic flexibility of TNBC MDA-MB-231 cells to generate subpopulations with glycolytic or oxidative phenotypes, we screened phenolic compounds containing an ortho-carbonyl group with mitochondrial activity and identified a bromoalkyl-ester of hydroquinone named FR58P1a, as a mitochondrial metabolism-affecting compound that uncouples OXPHOS through a protonophoric mechanism. In contrast to well-known protonophore uncoupler FCCP, FR58P1a does not depolarize the plasma membrane and its effect on the mitochondrial membrane potential and bioenergetics is moderate suggesting a mild uncoupling of OXPHOS. FR58P1a activates AMPK in a Sirt1-dependent fashion. Although the activation of Sirt1/AMPK axis by FR58P1a has a cyto-protective role, selectively inhibits

Materias

Multidisciplinary

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