Structure Analysis and Conformational Transitions of the Cell Penetrating Peptide Transportan 10 in the Membrane-Bound State

Structure analysis of the cell-penetrating peptide transportan 10 (TP10) revealed an exemplary range of different conformations in the membrane-bound state. The bipartite peptide (derived N-terminally from galanin and C-terminally from mastoparan) was found to exhibit prominent characteristics of (i...

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Autores principales: Fanghänel, Susanne, Wadhwani, Parvesh, Strandberg, Erik, Verdurmen, Wouter P. R., Bürck, Jochen, Ehni, Sebastian, Mykhailiuk, Pavel K., Afonin, Sergii, Gerthsen, Dagmar, Komarov, Igor V., Brock, Roland, Ulrich, Anne S.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4061077/
https://www.ncbi.nlm.nih.gov/pubmed/24937132
http://dx.doi.org/10.1371/journal.pone.0099653
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author Fanghänel, Susanne
Wadhwani, Parvesh
Strandberg, Erik
Verdurmen, Wouter P. R.
Bürck, Jochen
Ehni, Sebastian
Mykhailiuk, Pavel K.
Afonin, Sergii
Gerthsen, Dagmar
Komarov, Igor V.
Brock, Roland
Ulrich, Anne S.
author_facet Fanghänel, Susanne
Wadhwani, Parvesh
Strandberg, Erik
Verdurmen, Wouter P. R.
Bürck, Jochen
Ehni, Sebastian
Mykhailiuk, Pavel K.
Afonin, Sergii
Gerthsen, Dagmar
Komarov, Igor V.
Brock, Roland
Ulrich, Anne S.
author_sort Fanghänel, Susanne
collection PubMed
description Structure analysis of the cell-penetrating peptide transportan 10 (TP10) revealed an exemplary range of different conformations in the membrane-bound state. The bipartite peptide (derived N-terminally from galanin and C-terminally from mastoparan) was found to exhibit prominent characteristics of (i) amphiphilic α-helices, (ii) intrinsically disordered peptides, as well as (iii) β-pleated amyloid fibrils, and these conformational states become interconverted as a function of concentration. We used a complementary approach of solid-state (19)F-NMR and circular dichroism in oriented membrane samples to characterize the structural and dynamical behaviour of TP10 in its monomeric and aggregated forms. Nine different positions in the peptide were selectively substituted with either the L - or D -enantiomer of 3-(trifluoromethyl)-bicyclopent-[1.1.1]-1-ylglycine (CF(3) -Bpg) as a reporter group for (19)F-NMR. Using the L -epimeric analogs, a comprehensive three-dimensional structure analysis was carried out in lipid bilayers at low peptide concentration, where TP10 is monomeric. While the N-terminal region is flexible and intrinsically unstructured within the plane of the lipid bilayer, the C-terminal α-helix is embedded in the membrane with an oblique tilt angle of ∼55° and in accordance with its amphiphilic profile. Incorporation of the sterically obstructive D -CF(3) -Bpg reporter group into the helical region leads to a local unfolding of the membrane-bound peptide. At high concentration, these helix-destabilizing C-terminal substitutions promote aggregation into immobile β-sheets, which resemble amyloid fibrils. On the other hand, the obstructive D -CF(3) -Bpg substitutions can be accommodated in the flexible N-terminus of TP10 where they do not promote aggregation at high concentration. The cross-talk between the two regions of TP10 thus exerts a delicate balance on its conformational switch, as the presence of the α-helix counteracts the tendency of the unfolded N-terminus to self-assemble into β-pleated fibrils.
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spelling pubmed-40610772014-06-20 Structure Analysis and Conformational Transitions of the Cell Penetrating Peptide Transportan 10 in the Membrane-Bound State Fanghänel, Susanne Wadhwani, Parvesh Strandberg, Erik Verdurmen, Wouter P. R. Bürck, Jochen Ehni, Sebastian Mykhailiuk, Pavel K. Afonin, Sergii Gerthsen, Dagmar Komarov, Igor V. Brock, Roland Ulrich, Anne S. PLoS One Research Article Structure analysis of the cell-penetrating peptide transportan 10 (TP10) revealed an exemplary range of different conformations in the membrane-bound state. The bipartite peptide (derived N-terminally from galanin and C-terminally from mastoparan) was found to exhibit prominent characteristics of (i) amphiphilic α-helices, (ii) intrinsically disordered peptides, as well as (iii) β-pleated amyloid fibrils, and these conformational states become interconverted as a function of concentration. We used a complementary approach of solid-state (19)F-NMR and circular dichroism in oriented membrane samples to characterize the structural and dynamical behaviour of TP10 in its monomeric and aggregated forms. Nine different positions in the peptide were selectively substituted with either the L - or D -enantiomer of 3-(trifluoromethyl)-bicyclopent-[1.1.1]-1-ylglycine (CF(3) -Bpg) as a reporter group for (19)F-NMR. Using the L -epimeric analogs, a comprehensive three-dimensional structure analysis was carried out in lipid bilayers at low peptide concentration, where TP10 is monomeric. While the N-terminal region is flexible and intrinsically unstructured within the plane of the lipid bilayer, the C-terminal α-helix is embedded in the membrane with an oblique tilt angle of ∼55° and in accordance with its amphiphilic profile. Incorporation of the sterically obstructive D -CF(3) -Bpg reporter group into the helical region leads to a local unfolding of the membrane-bound peptide. At high concentration, these helix-destabilizing C-terminal substitutions promote aggregation into immobile β-sheets, which resemble amyloid fibrils. On the other hand, the obstructive D -CF(3) -Bpg substitutions can be accommodated in the flexible N-terminus of TP10 where they do not promote aggregation at high concentration. The cross-talk between the two regions of TP10 thus exerts a delicate balance on its conformational switch, as the presence of the α-helix counteracts the tendency of the unfolded N-terminus to self-assemble into β-pleated fibrils. Public Library of Science 2014-06-17 /pmc/articles/PMC4061077/ /pubmed/24937132 http://dx.doi.org/10.1371/journal.pone.0099653 Text en © 2014 Fanghänel et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Fanghänel, Susanne
Wadhwani, Parvesh
Strandberg, Erik
Verdurmen, Wouter P. R.
Bürck, Jochen
Ehni, Sebastian
Mykhailiuk, Pavel K.
Afonin, Sergii
Gerthsen, Dagmar
Komarov, Igor V.
Brock, Roland
Ulrich, Anne S.
Structure Analysis and Conformational Transitions of the Cell Penetrating Peptide Transportan 10 in the Membrane-Bound State
title Structure Analysis and Conformational Transitions of the Cell Penetrating Peptide Transportan 10 in the Membrane-Bound State
title_full Structure Analysis and Conformational Transitions of the Cell Penetrating Peptide Transportan 10 in the Membrane-Bound State
title_fullStr Structure Analysis and Conformational Transitions of the Cell Penetrating Peptide Transportan 10 in the Membrane-Bound State
title_full_unstemmed Structure Analysis and Conformational Transitions of the Cell Penetrating Peptide Transportan 10 in the Membrane-Bound State
title_short Structure Analysis and Conformational Transitions of the Cell Penetrating Peptide Transportan 10 in the Membrane-Bound State
title_sort structure analysis and conformational transitions of the cell penetrating peptide transportan 10 in the membrane-bound state
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4061077/
https://www.ncbi.nlm.nih.gov/pubmed/24937132
http://dx.doi.org/10.1371/journal.pone.0099653
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