Estrogen receptors (ERs) mediate the effects of 17b-estradiol under physiologic and pathologic conditions. ERs trigger 17bestradiol- sensitive gene transcription by binding to specific estrogen response elements (i.e. genomic mechanism). The cellular effects of estrogen are also influenced by membrane- or cytoplasm-initiated responses (i.e. nongenomic mechanism). Both ERevoked genomic and nongenomic effects originate from a unique signaling network. Furthermore, estrogen-initiated rapid pathways and ERa interactions with specific partners (e.g. AIB1, PELP1/MNAR; MTA1, MTA1s and p130Cas) influence both ER functions. Here, we summarize the recent findings related to multiple regulatory levels of the signaling networks responsible for ERs-mediated responses in breast cancer cells.
Acconcia, F., Kumar, R. (2006). Signaling regulation of genomic and nongenomic functions of estrogen receptors. CANCER LETTERS, 238, 1-14 [10.1016/j.canlet.2005.06.018].
Signaling regulation of genomic and nongenomic functions of estrogen receptors
ACCONCIA, FILIPPO;
2006-01-01
Abstract
Estrogen receptors (ERs) mediate the effects of 17b-estradiol under physiologic and pathologic conditions. ERs trigger 17bestradiol- sensitive gene transcription by binding to specific estrogen response elements (i.e. genomic mechanism). The cellular effects of estrogen are also influenced by membrane- or cytoplasm-initiated responses (i.e. nongenomic mechanism). Both ERevoked genomic and nongenomic effects originate from a unique signaling network. Furthermore, estrogen-initiated rapid pathways and ERa interactions with specific partners (e.g. AIB1, PELP1/MNAR; MTA1, MTA1s and p130Cas) influence both ER functions. Here, we summarize the recent findings related to multiple regulatory levels of the signaling networks responsible for ERs-mediated responses in breast cancer cells.I documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione.
