Literature DB >> 17535799

A conserved mechanism for steroid receptor translocation to the plasma membrane.

Ali Pedram1, Mahnaz Razandi, Richard C A Sainson, Jin K Kim, Christopher C Hughes, Ellis R Levin.   

Abstract

Multiple steroid receptors (SR) have been proposed to localize to the plasma membrane. Some structural elements for membrane translocation of the estrogen receptor alpha (ER alpha) have been described, but the mechanisms relevant to other steroid receptors are entirely unknown. Here, we identify a highly conserved 9 amino acid motif in the ligand binding domains (E domains) of human/mouse ER alpha and ER beta, progesterone receptors A and B, and the androgen receptor. Mutation of the phenylalanine or tyrosine at position-2, cysteine at position 0, and hydrophobic isoleucine/leucine or leucine/leucine combinations at positions +5/6, relative to cysteine, significantly reduced membrane localization, MAP and PI 3-kinase activation, thymidine incorporation into DNA, and cell viability, stimulated by specific SR ligands. The localization sequence mediated palmitoylation of each SR, which facilitated caveolin-1 association, subsequent membrane localization, and steroid signaling. Palmitoylation within the E domain is therefore a crucial modification for membrane translocation and function of classical sex steroid receptors.

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Year:  2007        PMID: 17535799     DOI: 10.1074/jbc.M611877200

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  187 in total

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Review 7.  Rapid effects of estrogens on behavior: environmental modulation and molecular mechanisms.

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10.  ERαΔ4, an ERα splice variant missing exon4, interacts with caveolin-3 and mGluR2/3.

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