Logo
Logo
Campo de búsqueda / búsqueda general

 
Autor
Título
Tema

Título: New insights into radioresistance in breast cancer identify a dual function of miR-122 as a tumor suppressor and oncomiR
Autor(es): PEREZ AÑORVE, ISIDRO XAVIER
GONZALEZ DE LA ROSA, CLAUDIA HAYDEE
SOTO REYES SOLIS, ERNESTO SOTO
BELTRAN ANAYA, FREDY OMAR
DEL MORAL HERNANDEZ, OSCAR
SALGADO ALBARRAN, MARISOL
ANGELES ZARAGOZA, OSCAR
GONZALEZ BARRIOS, JUAN ANTONIO
LANDERO HUERTA, DANIEL ADRIAN
CHAVEZ SALDAÑA, MARGARITA DOLORES
GARCIA CARRANCA, ALEJANDRO MANUEL
VILLEGAS SEPULVEDA, NICOLAS
ARECHAGA OCAMPO, ELENA
Temas: Cáncer de mama
MicroARN
miR-122
Radiorresistencia
Fecha: 2019
Editorial: Reino Unido : Wiley
Citation: Molecular Oncology 13, 5 (2019)
Resumen: Radioresistance of tumor cells gives rise to local recurrence and disease progression in many patients. MicroRNAs (miRNAs) are master regulators of gene expression that control oncogenic pathways to modulate the radiotherapy response of cells. In the present study, differential expression profiling assays identified 16 deregulated miRNAs in acquired radioresistant breast cancer cells, of which miR-122 was observed to be up-regulated. Functional analysis revealed that miR-122 has a role as a tumor suppressor in parental cells by decreasing survival and promoting radiosensitivity. However, in radioresistant cells, miR-122 functions as an oncomiR by promoting survival. The transcriptomic landscape resulting from knockdown of miR-122 in radioresistant cells showed modulation of the ZNF611, ZNF304, RIPK1, HRAS, DUSP8 and TNFRSF21 genes. Moreover, miR122 and the set of affected genes were prognostic factors in breast cancer patients treated with radiotherapy. Our data indicate that up-regulation of miR-122 promotes cell survival in acquired radioresistant breast cancer and also suggest that miR-122 differentially controls the response to radiotherapy by a dual function as a tumor suppressor an and oncomiR dependent on cell phenotype.
URI: http://ilitia.cua.uam.mx:8080/jspui/handle/123456789/847
Aparece en las colecciones:Artículos



Items in DSpace are protected by copyright, with all rights reserved, unless otherwise indicated.