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Endocrinology Vol. 144, No. 7 2967-2976
Copyright © 2003 by The Endocrine Society

The Naturally Occurring Variant of Estrogen Receptor (ER) ER{Delta}E7 Suppresses Estrogen-Dependent Transcriptional Activation by Both Wild-Type ER{alpha} and ERß

Juana M. García Pedrero, Pedro Zuazua, Carlos Martínez-Campa, Pedro S. Lazo and Sofía Ramos

Departamento de Bioquímica y Biología Molecular, Instituto Universitario de Oncología Principado de Asturias, Universidad de Oviedo, 33071 Oviedo, Spain

Address all correspondence and requests for reprints to: S. Ramos, Departamento de Bioquímica y Biología Molecular, Instituto Universitario de Oncología Principado de Asturias, Universidad de Oviedo, 33071 Oviedo, Spain. E-mail: sramos{at}correo.uniovi.es.

We have isolated and functionally characterized the exon 7-skipped variant (ER{Delta}E7) of estrogen receptor (ER){alpha}, which has emerged as the predominant variant expressed in multiple normal and tumoral tissues. However, to date no function has been established for this variant in mammalian cells. ER{Delta}E7 exhibits a negligible ability to bind ligands, insensitivity to allosteric modulation by estrogen and antiestrogens, and loss of estrogen-dependent interaction with p160 coactivators such as SRC-1 and AIB1. ER{Delta}E7 is able to form heterodimers with both ER{alpha} and ERß in a ligand-independent manner. Transient expression experiments in HeLa cells show that increasing amounts of ER{Delta}E7 result in a progressive inhibition of the estrogen-dependent transcriptional activation by both wild-type ER{alpha} and ERß on estrogen response element-driven promoters. The inhibitory effect of ER{Delta}E7 is due to the inhibition of binding of wild-type receptors to their responsive elements. Surprisingly, the activation function (AF)-1-dependent transactivation triggered by epithelial growth factor and phorbol-12-myristate-13-acetate is also abolished in ER{Delta}E7 despite AF1 integrity, suggesting a cross-talk between AF1 and AF2 regions of the receptor. These results indicate that the naturally occurring variant ER{Delta}E7 is a dominant negative receptor that, when expressed at high levels relative to wild-type ERs, might have profound effects on several estrogen-dependent functions.




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