1997
DOI: 10.1074/jbc.272.17.11384
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Estrogen Receptor Ligands Modulate Its Interaction with DNA

Abstract: The estrogen receptor (ER) belongs to a superfamily of ligand-inducible transcription factors. Functions of these proteins (dimerization, DNA binding, and interaction with other transcription factors) are modulated by binding of their corresponding ligands. It is, however, controversial whether various ER ligands affect the receptor's ability to bind its specific DNA element (ERE).By using real time interaction analysis we have investigated the kinetics of human (h)ER binding to DNA in the absence and presence… Show more

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Cited by 119 publications
(87 citation statements)
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“…4). These findings are generally consistent with the results of previous experiments on the binding of ER (in the absence of associated heat shock proteins) to naked DNA in vitro (see, e.g., Murdoch et al 1990;Furlow et al 1993;Metzger et al 1995;Cheskis et al 1997). We do not, however, extrapolate these data to the behavior of ER in vivo, as these experiments with free polypeptide ER do not involve issues such as the association of heat shock proteins with ER and nuclear localization.…”
Section: Relation Between Binding Of Er To Chromatin and Transcriptiosupporting
confidence: 92%
“…4). These findings are generally consistent with the results of previous experiments on the binding of ER (in the absence of associated heat shock proteins) to naked DNA in vitro (see, e.g., Murdoch et al 1990;Furlow et al 1993;Metzger et al 1995;Cheskis et al 1997). We do not, however, extrapolate these data to the behavior of ER in vivo, as these experiments with free polypeptide ER do not involve issues such as the association of heat shock proteins with ER and nuclear localization.…”
Section: Relation Between Binding Of Er To Chromatin and Transcriptiosupporting
confidence: 92%
“…However, binding of oestradiol to the ER initiates a cascade of events leading to strong ER dimerisation, increased nuclear localisation and binding to ERE in the regulatory regions of target genes, and gene transcription (mediated by AF1 and AF2 of the ER) (Beato 1989, Tsai & O'Malley 1994, Cheskis et al 1997. AF1 (located in domains A and B of the amino terminal of the ER) is activated by growth factors acting through the mitogen-activated protein kinase (MAPK) pathway, while AF2 (located in domain E of the carboxy terminal of the ER ligandbinding domain) is activated by oestradiol.…”
Section: Classical Pathway Of Er Signallingmentioning
confidence: 99%
“…Raloxifene binds both ERa and ERb (Glasebrook et al 1993, Gize et al 1997, and the importance of ERs for the physiological effects of raloxifene has been demonstrated in various cell types using the selective ER antagonist ICI182.780 (Ashby et al 1997, Viereck et al 2003. The interaction between raloxifene and ER causes structural differences in the complex compared with the oestrogen-ER complex (Bryant et al 1999), and these structural differences result in assembly of other coregulators (Cheskis et al 1997), which causes the tissue-specific agonistic/antagonistic effects of raloxifene.…”
Section: Introductionmentioning
confidence: 99%