SPBP Is a Phosphoserine-Specific Repressor of Estrogen Receptor α

Author:

Gburcik Valentina1,Bot Nathalie1,Maggiolini Marcello2,Picard Didier1

Affiliation:

1. Département de Biologie Cellulaire, Université de Genève, Sciences III, Geneva, Switzerland

2. Department of Pharmaco-Biology, University of Calabria, Rende (CS), Italy

Abstract

ABSTRACT Multiple signaling pathways stimulate the activity of estrogen receptor α (ERα) by direct phosphorylation within its N-terminal activation function 1 (AF1). How phosphorylation affects AF1 activity remains poorly understood. We performed a phage display screen for human proteins that are exclusively recruited to the phosphorylated form of AF1 and found the stromelysin-1 platelet-derived growth factor-responsive element-binding protein (SPBP). In a purified system, SPBP bound only the in vitro-phosphorylated form of the ERα AF1 or the phosphoserine mimic S118E, and the interaction domain could be mapped to a 42-amino-acid fragment of SPBP. In cells, SPBP preferentially interacted with liganded and phosphorylated ERα. Functionally, SPBP behaved as a repressor of activated ERα, which extends its previously demonstrated roles as a DNA binding transactivation factor and coactivator of other transcription factors. By targeting the phosphorylated form of AF1, SPBP may contribute to attenuating and fine-tuning ERα activity. A functional consequence is that SPBP inhibits the proliferation of ERα-dependent but not ERα-independent breast cancer cell lines, mirroring a reported negative correlation with the ERα status of breast tumors.

Publisher

American Society for Microbiology

Subject

Cell Biology,Molecular Biology

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