Interaction of Transcriptional Intermediary Factor 2 Nuclear Receptor Box Peptides with the Coactivator Binding Site of Estrogen Receptor α

Wärnmark, Anette; Treuter, Eckardt; Gustafsson, Jan‐Åke; Hubbard, Roderick E.; Brzozowski, A.M.; Pike, Ashley C.W.

doi:10.1074/jbc.m200764200

Cited by 154 publications

(171 citation statements)

References 38 publications

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“…In fact, the crystal structures of PGC-1␣ NR3 displayed the right orientation of the LXXYL motif when it binds to ERR␣ (40,41). A similar finding was made with an LXXYL motif from another NR coactivator when the crystal structure of SRC2 NR3 in complex with ER␣ displayed the LXXYL motif in right orientation (71). Fur-FIGURE 6.…”

Section: Discussionsupporting

confidence: 62%

Multiple Binding Modes between HNF4α and the LXXLL Motifs of PGC-1α Lead to Full Activation

Rha

Shoelson

et al. 2009

Journal of Biological Chemistry

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Hepatocyte nuclear factor 4␣ (HNF4␣) is a novel nuclear receptor that participates in a hierarchical network of transcription factors regulating the development and physiology of such vital organs as the liver, pancreas, and kidney. Among the various transcriptional coregulators with which HNF4␣ interacts, peroxisome proliferation-activated receptor ␥ (PPAR␥) coactivator 1␣ (PGC-1␣) represents a novel coactivator whose activation is unusually robust and whose binding mode appears to be distinct from that of canonical coactivators such as NCoA/SRC/ p160 family members. To elucidate the potentially unique molecular mechanism of PGC-1␣ recruitment, we have determined the crystal structure of HNF4␣ in complex with a fragment of PGC-1␣ containing all three of its LXXLL motifs. Despite the presence of all three LXXLL motifs available for interactions, only one is bound at the canonical binding site, with no additional contacts observed between the two proteins. However, a close inspection of the electron density map indicates that the bound LXXLL motif is not a selected one but an averaged structure of more than one LXXLL motif. Further biochemical and functional studies show that the individual LXXLL motifs can bind but drive only minimal transactivation. Only when more than one LXXLL motif is involved can significant transcriptional activity be measured, and full activation requires all three LXXLL motifs. These findings led us to propose a model wherein each LXXLL motif has an additive effect, and the multiple binding modes by HNF4␣ toward the LXXLL motifs of PGC-1␣ could account for the apparent robust activation by providing a flexible mechanism for combinatorial recruitment of additional coactivators and mediators.

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Section: Discussionsupporting

confidence: 62%

Multiple Binding Modes between HNF4α and the LXXLL Motifs of PGC-1α Lead to Full Activation

Rha

Shoelson

et al. 2009

Journal of Biological Chemistry

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“…This view is supported by studies of short peptides containing a single NR box reporting preferential binding of specific NR boxes to NRs (14)(15)(16). However, such studies neglect the influence of protein conformation on binding (17). We demonstrated that eliminating NR box III by truncating SRC1NID changes the binding properties in a nontrivial way.…”

Section: Discussionmentioning

confidence: 70%

Determining the stoichiometry of protein heterocomplexes in living cells with fluorescence fluctuation spectroscopy

Chen

Müller²

2007

Proc. Natl. Acad. Sci. U.S.A.

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FFS is an attractive candidate for studying protein interactions in cells and is based on fluctuations in the fluorescence intensity observed in a small observation volume (Ͻ1 fl) that are due to individual proteins entering or leaving the volume (1). Fluorescence correlation spectroscopy (FCS) uses correlation functions to determine the concentration and temporal properties of proteins, and dual-color FCS has been used to detect protein interactions in cells (2, 3). However, a quantitative characterization of protein interactions has proven to be difficult. We argued previously that brightness analysis of fluctuations is a promising method for quantifying protein interactions in living cells (4). The brightness of a molecule is defined as the average fluorescence intensity of a single particle, and analysis methods that determine the brightness from fluctuation data are available (5, 6).Brightness encodes the stoichiometry of protein complexes. Consider the case of a dimer. If the monomeric protein carries a fluorescent protein of brightness then the homodimer exhibits a brightness of 2 , because it carries two fluorophores. This concept was experimentally verified by using GFP as a marker and applied to study the concentration-dependent dimerization of nuclear receptors (NRs) in living cells (7). However, the use of a single fluorescent color limits brightness analysis to homocomplex formation. Two fluorescent colors are required to tackle heterointeractions. We developed the analysis tools for brightness analysis of two colors and tested it by using the heterodimer of the ligand-binding domains (LBD) of the NRs retinoic X receptor (RXR) and retinoic acid receptor (RAR) in CV-1 cells (8). Quantifying heterointeractions is considerably more complex than the analysis of homocomplex formation, and a method that identifies a heterocomplex of unknown composition is currently unavailable. In this manuscript we devise a methodology that solves this problem and identifies the stoichiometry of two proteins labeled with CFP and YFP within a cellular protein complex. We also introduce the brightness profile, which characterizes the normalized brightness as a function of the coexpression ratio of the labeled proteins. The brightness profile is used together with brightness titration experiments to deduce the composition of a protein complex at stoichiometric binding conditions. We illustrate the method using a protein complex that is larger than a dimer to highlight the inherent strength of brightness analysis.NRs such as RXR are known to interact with coactivators. It is generally thought that two NRs bind a single coactivator molecule, thus providing a suitable test system that goes beyond the simple dimer model. We choose the LBD of RXR and the NR interacting domain (NID) of SRC1 (steroid receptor coactivator 1) as a minimal model for exploring the formation of a hetero-oligomer by FFS directly in living cells. Brightness analysis revealed that RXRLBD and SRC1NID form a heterotetramer with three RXRLBDs binding to one ...

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“…By a computer-based protein modeling approach , we recently identified a putative regulatory intramolecular interaction between a motif included in the P295-T311 sequence (aa 301-311) and the helix H4 which is located within a region known to recruit co-regulators (H3-H5) (Warnmark et al, 2002;Kong et al, 2005). Hence, the estrogen-like activity of ERa17p might stem from its ability to interfere with this regulatory mechanism.…”

Section: Discussionmentioning

confidence: 99%

Calmodulin-independent, agonistic properties of a peptide containing the calmodulin binding site of estrogen receptor α

Gallo

Jacquemotte²,

Cleeren

et al. 2007

Molecular and Cellular Endocrinology

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Interaction of Transcriptional Intermediary Factor 2 Nuclear Receptor Box Peptides with the Coactivator Binding Site of Estrogen Receptor α

Cited by 154 publications

References 38 publications

Multiple Binding Modes between HNF4α and the LXXLL Motifs of PGC-1α Lead to Full Activation

Multiple Binding Modes between HNF4α and the LXXLL Motifs of PGC-1α Lead to Full Activation

Determining the stoichiometry of protein heterocomplexes in living cells with fluorescence fluctuation spectroscopy

Calmodulin-independent, agonistic properties of a peptide containing the calmodulin binding site of estrogen receptor α

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