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Please use this identifier to cite or link to this item: http://acervodigital.unesp.br/handle/11449/72253
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dc.contributor.authorFigueira, A. C M-
dc.contributor.authorSaidemberg, D. M.-
dc.contributor.authorSouza, P. C T-
dc.contributor.authorMartínez, L.-
dc.contributor.authorScanlan, T. S.-
dc.contributor.authorBaxter, J. D.-
dc.contributor.authorSkaf, M. S.-
dc.contributor.authorPalma, Mario Sergio-
dc.contributor.authorWebb, P.-
dc.contributor.authorPolikarpov, I.-
dc.date.accessioned2014-05-27T11:25:26Z-
dc.date.accessioned2016-10-25T18:33:28Z-
dc.date.available2014-05-27T11:25:26Z-
dc.date.available2016-10-25T18:33:28Z-
dc.date.issued2011-01-01-
dc.identifierhttp://dx.doi.org/10.1210/me.2010-0202-
dc.identifier.citationMolecular Endocrinology, v. 25, n. 1, p. 15-31, 2011.-
dc.identifier.issn0888-8809-
dc.identifier.urihttp://hdl.handle.net/11449/72253-
dc.identifier.urihttp://acervodigital.unesp.br/handle/11449/72253-
dc.description.abstractThyroid hormone receptors (TRs) are ligand-gated transcription factors with critical roles in development and metabolism. Although x-ray structures of TR ligand-binding domains (LBDs) with agonists are available, comparable structures without ligand (apo-TR) or with antagonists are not. It remains important to understand apo-LBD conformation and the way that it rearranges with ligands to develop better TR pharmaceuticals. In this study, we conducted hydrogen/deuterium exchange on TR LBDs with or without agonist (T 3) or antagonist (NH3). Both ligands reduce deuterium incorporation into LBD amide hydrogens, implying tighter overall folding of the domain. As predicted, mass spectroscopic analysis of individual proteolytic peptides after hydrogen/ deuterium exchange reveals that ligand increases the degree of solvent protection of regions close to the buried ligand-binding pocket. However, there is also extensive ligand protection of other regions, including the dimer surface at H10-H11, providing evidence for allosteric communication between the ligand-binding pocket and distant interaction surfaces. Surprisingly, Cterminal activation helix H12, which is known to alter position with ligand, remains relatively protected from solvent in all conditions suggesting that it is packed against the LBD irrespective of the presence or type of ligand. T 3, but not NH3, increases accessibility of the upper part of H3-H5 to solvent, and we propose that TR H12 interacts with this region in apo-TR and that this interaction is blocked by T 3 but not NH3.Wepresent data from site-directed mutagenesis experiments and molecular dynamics simulations that lend support to this structural model of apo-TR and its ligand-dependent conformational changes. (Molecular Endocrinology 25: 15-31, 2011). Copyright © 2011 by The Endocrine Society.en
dc.format.extent15-31-
dc.language.isoeng-
dc.sourceScopus-
dc.subjectamide-
dc.subjectammonia-
dc.subjectbinding protein-
dc.subjectdeuterium-
dc.subjectdimer-
dc.subjecthormone receptor affecting agent-
dc.subjecthormone receptor blocking agent-
dc.subjecthydrogen-
dc.subjectligand-
dc.subjectligand binding protein-
dc.subjectpeptide-
dc.subjectsolvent-
dc.subjectthyroid hormone receptor-
dc.subjectthyroid hormone receptor agonist-
dc.subjectthyroid hormone receptor antagonist-
dc.subjectunclassified drug-
dc.subjectallosterism-
dc.subjectcarboxy terminal sequence-
dc.subjectcontrolled study-
dc.subjectdeuterium hydrogen exchange-
dc.subjectdimerization-
dc.subjectfemale-
dc.subjecthuman-
dc.subjecthuman cell-
dc.subjectligand binding-
dc.subjectmass spectrometry-
dc.subjectpriority journal-
dc.subjectprotein conformation-
dc.subjectprotein degradation-
dc.subjectprotein domain-
dc.subjectprotein expression-
dc.subjectprotein function-
dc.subjectprotein protein interaction-
dc.subjectsurface property-
dc.subjectAmino Acid Sequence-
dc.subjectAmmonia-
dc.subjectApoproteins-
dc.subjectDeuterium-
dc.subjectDeuterium Exchange Measurement-
dc.subjectHumans-
dc.subjectLigands-
dc.subjectMolecular Dynamics Simulation-
dc.subjectMolecular Sequence Data-
dc.subjectMutation-
dc.subjectPeptides-
dc.subjectProtein Structure, Secondary-
dc.subjectProtein Structure, Tertiary-
dc.subjectReceptors, Thyroid Hormone-
dc.subjectSequence Alignment-
dc.subjectSolvents-
dc.subjectTriiodothyronine-
dc.titleAnalysis of agonist and antagonist effects on thyroid hormone receptor conformation by hydrogen/deuterium exchangeen
dc.typeoutro-
dc.contributor.institutionUniversidade de São Paulo (USP)-
dc.contributor.institutionLaboratoacute;rio Nacional de Biociências-
dc.contributor.institutionUniversidade Estadual Paulista (UNESP)-
dc.contributor.institutionUniversidade Estadual de Campinas (UNICAMP)-
dc.contributor.institutionOregon Health and Science University-
dc.contributor.institutionMethodist Hospital Research Institute-
dc.description.affiliationLaboratório de Cristalografia de Proteías Instituto de Física de São Carlos Universidade de São Paulo, São Carlos, SP, 13560-970-
dc.description.affiliationLaboratoacute;rio Nacional de Biociências, Campinas, SP, 13083-100-
dc.description.affiliationDepartamento de Biologia Centro de Estudos de Insetos Sociais - Instituto de Biociências de Rio Claro Universidade Estadual Paulista, Rio Claro, SP, 13506-900-
dc.description.affiliationInstitute of Chemistry State University of Campinas, Campinas, SP, 13083-970-
dc.description.affiliationDepartment of Physiology and Pharmacology Oregon Health and Science University, Portland, OR-
dc.description.affiliationDiabetes Center and Cancer Research Unit Methodist Hospital Research Institute, Houston, TX 77030-
dc.description.affiliationUnespDepartamento de Biologia Centro de Estudos de Insetos Sociais - Instituto de Biociências de Rio Claro Universidade Estadual Paulista, Rio Claro, SP, 13506-900-
dc.identifier.doi10.1210/me.2010-0202-
dc.rights.accessRightsAcesso restrito-
dc.relation.ispartofMolecular Endocrinology-
dc.identifier.scopus2-s2.0-78650854003-
Appears in Collections:Artigos, TCCs, Teses e Dissertações da Unesp

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