The peripheral binding of 14-3-3γ to membranes involves isoform-specific histidine residues.

The peripheral binding of 14-3-3γ to membranes involves isoform-specific histidine residues.

Mammalian 14-3-3 protein scaffolds include seven conserved isoforms that bind numerous phosphorylated protein partners and regulate many cellular processes. Some 14-3-3-isoforms, notably γ, have elevated affinity for membranes, which might contribute to modulate the subcellular localization of the p...

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Main Authors: Helene J Bustad, Lars Skjaerven, Ming Ying, Øyvind Halskau, Anne Baumann, David Rodriguez-Larrea, Miguel Costas, Jarl Underhaug, Jose M Sanchez-Ruiz, Aurora Martinez
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2012-01-01
Series:PLoS ONE
Online Access:https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/23189152/?tool=EBI
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spelling doaj-0bbdece711e542388e84f0510ac609202021-03-04T00:00:35ZengPublic Library of Science (PLoS)PLoS ONE1932-62032012-01-01711e4967110.1371/journal.pone.0049671The peripheral binding of 14-3-3γ to membranes involves isoform-specific histidine residues.Helene J BustadLars SkjaervenMing YingØyvind HalskauAnne BaumannDavid Rodriguez-LarreaMiguel CostasJarl UnderhaugJose M Sanchez-RuizAurora MartinezMammalian 14-3-3 protein scaffolds include seven conserved isoforms that bind numerous phosphorylated protein partners and regulate many cellular processes. Some 14-3-3-isoforms, notably γ, have elevated affinity for membranes, which might contribute to modulate the subcellular localization of the partners and substantiate the importance of investigating molecular mechanisms of membrane interaction. By applying surface plasmon resonance we here show that the binding to phospholipid bilayers is stimulated when 14-3-3γ is complexed with its partner, a peptide corresponding to the Ser19-phosphorylated N-terminal region of tyrosine hydroxylase. Moreover, membrane interaction is dependent on salts of kosmotropic ions, which also stabilize 14-3-3γ. Electrostatic analysis of available crystal structures of γ and of the non-membrane-binding ζ-isoform, complemented with molecular dynamics simulations, indicate that the electrostatic potential distribution of phosphopeptide-bound 14-3-3γ is optimal for interaction with the membrane through amphipathic helices at the N-terminal dimerization region. In addition, His158, and especially His195, both specific to 14-3-3γ and located at the convex lateral side, appeared to be pivotal for the ligand induced membrane interaction, as corroborated by site-directed mutagenesis. The participation of these histidine residues might be associated to their increased protonation upon membrane binding. Overall, these results reveal membrane-targeting motifs and give insights on mechanisms that furnish the 14-3-3γ scaffold with the capacity for tuned shuffling from soluble to membrane-bound states.https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/23189152/?tool=EBI
collection DOAJ
language English
format Article
sources DOAJ
author Helene J Bustad
Lars Skjaerven
Ming Ying
Øyvind Halskau
Anne Baumann
David Rodriguez-Larrea
Miguel Costas
Jarl Underhaug
Jose M Sanchez-Ruiz
Aurora Martinez
spellingShingle Helene J Bustad
Lars Skjaerven
Ming Ying
Øyvind Halskau
Anne Baumann
David Rodriguez-Larrea
Miguel Costas
Jarl Underhaug
Jose M Sanchez-Ruiz
Aurora Martinez
The peripheral binding of 14-3-3γ to membranes involves isoform-specific histidine residues.
PLoS ONE
author_facet Helene J Bustad
Lars Skjaerven
Ming Ying
Øyvind Halskau
Anne Baumann
David Rodriguez-Larrea
Miguel Costas
Jarl Underhaug
Jose M Sanchez-Ruiz
Aurora Martinez
author_sort Helene J Bustad
title The peripheral binding of 14-3-3γ to membranes involves isoform-specific histidine residues.
title_short The peripheral binding of 14-3-3γ to membranes involves isoform-specific histidine residues.
title_full The peripheral binding of 14-3-3γ to membranes involves isoform-specific histidine residues.
title_fullStr The peripheral binding of 14-3-3γ to membranes involves isoform-specific histidine residues.
title_full_unstemmed The peripheral binding of 14-3-3γ to membranes involves isoform-specific histidine residues.
title_sort peripheral binding of 14-3-3γ to membranes involves isoform-specific histidine residues.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2012-01-01
description Mammalian 14-3-3 protein scaffolds include seven conserved isoforms that bind numerous phosphorylated protein partners and regulate many cellular processes. Some 14-3-3-isoforms, notably γ, have elevated affinity for membranes, which might contribute to modulate the subcellular localization of the partners and substantiate the importance of investigating molecular mechanisms of membrane interaction. By applying surface plasmon resonance we here show that the binding to phospholipid bilayers is stimulated when 14-3-3γ is complexed with its partner, a peptide corresponding to the Ser19-phosphorylated N-terminal region of tyrosine hydroxylase. Moreover, membrane interaction is dependent on salts of kosmotropic ions, which also stabilize 14-3-3γ. Electrostatic analysis of available crystal structures of γ and of the non-membrane-binding ζ-isoform, complemented with molecular dynamics simulations, indicate that the electrostatic potential distribution of phosphopeptide-bound 14-3-3γ is optimal for interaction with the membrane through amphipathic helices at the N-terminal dimerization region. In addition, His158, and especially His195, both specific to 14-3-3γ and located at the convex lateral side, appeared to be pivotal for the ligand induced membrane interaction, as corroborated by site-directed mutagenesis. The participation of these histidine residues might be associated to their increased protonation upon membrane binding. Overall, these results reveal membrane-targeting motifs and give insights on mechanisms that furnish the 14-3-3γ scaffold with the capacity for tuned shuffling from soluble to membrane-bound states.
url https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/23189152/?tool=EBI
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