Importance of the Sequence-Directed DNA Shape for Specific Binding Site Recognition by the Estrogen-Related Receptor

Most nuclear receptors (NRs) bind DNA as dimers, either as hetero- or as homodimers on DNA sequences organized as two half-sites with specific orientation and spacing. The dimerization of NRs on their cognate response elements (REs) involves specific protein–DNA and protein–protein interactions. The...

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Autores principales: Mohideen-Abdul, Kareem, Tazibt, Karima, Bourguet, Maxime, Hazemann, Isabelle, Lebars, Isabelle, Takacs, Maria, Cianférani, Sarah, Klaholz, Bruno P., Moras, Dino, Billas, Isabelle M. L.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2017
Materias:
Endocrinology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5476932/
https://www.ncbi.nlm.nih.gov/pubmed/28676789
http://dx.doi.org/10.3389/fendo.2017.00140
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author Mohideen-Abdul, Kareem
Tazibt, Karima
Bourguet, Maxime
Hazemann, Isabelle
Lebars, Isabelle
Takacs, Maria
Cianférani, Sarah
Klaholz, Bruno P.
Moras, Dino
Billas, Isabelle M. L.
author_facet Mohideen-Abdul, Kareem
Tazibt, Karima
Bourguet, Maxime
Hazemann, Isabelle
Lebars, Isabelle
Takacs, Maria
Cianférani, Sarah
Klaholz, Bruno P.
Moras, Dino
Billas, Isabelle M. L.
author_sort Mohideen-Abdul, Kareem
collection PubMed
description Most nuclear receptors (NRs) bind DNA as dimers, either as hetero- or as homodimers on DNA sequences organized as two half-sites with specific orientation and spacing. The dimerization of NRs on their cognate response elements (REs) involves specific protein–DNA and protein–protein interactions. The estrogen-related receptor (ERR) belongs to the steroid hormone nuclear receptor (SHR) family and shares strong similarity in its DNA-binding domain (DBD) with that of the estrogen receptor (ER). In vitro, ERR binds with high affinity inverted repeat REs with a 3-bps spacing (IR3), but in vivo, it preferentially binds to single half-site REs extended at the 5′-end by 3 bp [estrogen-related response element (ERREs)], thus explaining why ERR was often inferred as a purely monomeric receptor. Since its C-terminal ligand-binding domain is known to homodimerize with a strong dimer interface, we investigated the binding behavior of the isolated DBDs to different REs using electrophoretic migration, multi-angle static laser light scattering (MALLS), non-denaturing mass spectrometry, and nuclear magnetic resonance. In contrast to ER DBD, ERR DBD binds as a monomer to EREs (IR3), such as the tff1 ERE-IR3, but we identified a DNA sequence composed of an extended half-site embedded within an IR3 element (embedded ERRE/IR3), where stable dimer binding is observed. Using a series of chimera and mutant DNA sequences of ERREs and IR3 REs, we have found the key determinants for the binding of ERR DBD as a dimer. Our results suggest that the sequence-directed DNA shape is more important than the exact nucleotide sequence for the binding of ERR DBD to DNA as a dimer. Our work underlines the importance of the shape-driven DNA readout mechanisms based on minor groove recognition and electrostatic potential. These conclusions may apply not only to ERR but also to other members of the SHR family, such as androgen or glucocorticoid, for which a strong well-conserved half-site is followed by a weaker one with degenerated sequence.
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spelling pubmed-54769322017-07-04 Importance of the Sequence-Directed DNA Shape for Specific Binding Site Recognition by the Estrogen-Related Receptor Mohideen-Abdul, Kareem Tazibt, Karima Bourguet, Maxime Hazemann, Isabelle Lebars, Isabelle Takacs, Maria Cianférani, Sarah Klaholz, Bruno P. Moras, Dino Billas, Isabelle M. L. Front Endocrinol (Lausanne) Endocrinology Most nuclear receptors (NRs) bind DNA as dimers, either as hetero- or as homodimers on DNA sequences organized as two half-sites with specific orientation and spacing. The dimerization of NRs on their cognate response elements (REs) involves specific protein–DNA and protein–protein interactions. The estrogen-related receptor (ERR) belongs to the steroid hormone nuclear receptor (SHR) family and shares strong similarity in its DNA-binding domain (DBD) with that of the estrogen receptor (ER). In vitro, ERR binds with high affinity inverted repeat REs with a 3-bps spacing (IR3), but in vivo, it preferentially binds to single half-site REs extended at the 5′-end by 3 bp [estrogen-related response element (ERREs)], thus explaining why ERR was often inferred as a purely monomeric receptor. Since its C-terminal ligand-binding domain is known to homodimerize with a strong dimer interface, we investigated the binding behavior of the isolated DBDs to different REs using electrophoretic migration, multi-angle static laser light scattering (MALLS), non-denaturing mass spectrometry, and nuclear magnetic resonance. In contrast to ER DBD, ERR DBD binds as a monomer to EREs (IR3), such as the tff1 ERE-IR3, but we identified a DNA sequence composed of an extended half-site embedded within an IR3 element (embedded ERRE/IR3), where stable dimer binding is observed. Using a series of chimera and mutant DNA sequences of ERREs and IR3 REs, we have found the key determinants for the binding of ERR DBD as a dimer. Our results suggest that the sequence-directed DNA shape is more important than the exact nucleotide sequence for the binding of ERR DBD to DNA as a dimer. Our work underlines the importance of the shape-driven DNA readout mechanisms based on minor groove recognition and electrostatic potential. These conclusions may apply not only to ERR but also to other members of the SHR family, such as androgen or glucocorticoid, for which a strong well-conserved half-site is followed by a weaker one with degenerated sequence. Frontiers Media S.A. 2017-06-20 /pmc/articles/PMC5476932/ /pubmed/28676789 http://dx.doi.org/10.3389/fendo.2017.00140 Text en Copyright © 2017 Mohideen-Abdul, Tazibt, Bourguet, Hazemann, Lebars, Takacs, Cianférani, Klaholz, Moras and Billas. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) or licensor are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Endocrinology
Mohideen-Abdul, Kareem
Tazibt, Karima
Bourguet, Maxime
Hazemann, Isabelle
Lebars, Isabelle
Takacs, Maria
Cianférani, Sarah
Klaholz, Bruno P.
Moras, Dino
Billas, Isabelle M. L.
Importance of the Sequence-Directed DNA Shape for Specific Binding Site Recognition by the Estrogen-Related Receptor
title Importance of the Sequence-Directed DNA Shape for Specific Binding Site Recognition by the Estrogen-Related Receptor
title_full Importance of the Sequence-Directed DNA Shape for Specific Binding Site Recognition by the Estrogen-Related Receptor
title_fullStr Importance of the Sequence-Directed DNA Shape for Specific Binding Site Recognition by the Estrogen-Related Receptor
title_full_unstemmed Importance of the Sequence-Directed DNA Shape for Specific Binding Site Recognition by the Estrogen-Related Receptor
title_short Importance of the Sequence-Directed DNA Shape for Specific Binding Site Recognition by the Estrogen-Related Receptor
title_sort importance of the sequence-directed dna shape for specific binding site recognition by the estrogen-related receptor
topic Endocrinology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5476932/
https://www.ncbi.nlm.nih.gov/pubmed/28676789
http://dx.doi.org/10.3389/fendo.2017.00140
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