Estrogen Dendrimer Conjugates That Preferentially Activate Extranuclear, Nongenomic Versus Genomic Pathways of Estrogen Action

Overview

Journal Mol Endocrinol

Specialties Endocrinology
Molecular Biology

Date 2005 Nov 25

PMID 16306086

Citations 129

Authors

William R Harrington

Sung Hoon Kim

Cory C Funk

Zeynep Madak-Erdogan

Rachel Schiff

John A Katzenellenbogen

Benita S Katzenellenbogen

Affiliations

Soon will be listed here.

Abstract

Estrogenic hormones are classically thought to exert their effects by binding to nuclear estrogen receptors and altering target gene transcription, but estrogens can also have nongenomic effects through rapid activation of membrane-initiated kinase cascades. The development of ligands that selectively activate only the nongenomic pathways would provide useful tools to investigate the significance of these pathways. We have prepared large, abiotic, nondegradable poly(amido)amine dendrimer macromolecules that are conjugated to multiple estrogen molecules through chemically robust linkages. Because of their charge and size, these estrogen-dendrimer conjugates (EDCs) remain outside the nucleus. They stimulate ERK, Shc, and Src phosphorylation in MCF-7 breast cancer cells at low concentrations, yet they are very ineffective in stimulating transcription of endogenous estrogen target genes, being approximately 10,000-fold less potent than estradiol in genomic actions. In contrast to estradiol, EDC was not effective in stimulating breast cancer cell proliferation. Because these EDC ligands activate nongenomic activity at concentrations at which they do not alter the transcription of estrogen target genes, they should be useful in studying extranuclear initiated pathways of estrogen action in a variety of target cells.

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