A Synchrotron-Based Hydroxyl Radical Footprinting Analysis of Amyloid Fibrils and Prefibrillar Intermediates with Residue-Specific Resolution

[Image: see text] Structural models of the fibrils formed by the 40-residue amyloid-β (Aβ40) peptide in Alzheimer’s disease typically consist of linear polypeptide segments, oriented approximately perpendicular to the long axis of the fibril, and joined together as parallel in-register β-sheets to f...

Descripción completa

Detalles Bibliográficos
Autores principales: Klinger, Alexandra L., Kiselar, Janna, Ilchenko, Serguei, Komatsu, Hiroaki, Chance, Mark R., Axelsen, Paul H.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Chemical Society 2014
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4270378/
https://www.ncbi.nlm.nih.gov/pubmed/25382225
http://dx.doi.org/10.1021/bi5010409
_version_ 1782349483527372800
author Klinger, Alexandra L.
Kiselar, Janna
Ilchenko, Serguei
Komatsu, Hiroaki
Chance, Mark R.
Axelsen, Paul H.
author_facet Klinger, Alexandra L.
Kiselar, Janna
Ilchenko, Serguei
Komatsu, Hiroaki
Chance, Mark R.
Axelsen, Paul H.
author_sort Klinger, Alexandra L.
collection PubMed
description [Image: see text] Structural models of the fibrils formed by the 40-residue amyloid-β (Aβ40) peptide in Alzheimer’s disease typically consist of linear polypeptide segments, oriented approximately perpendicular to the long axis of the fibril, and joined together as parallel in-register β-sheets to form filaments. However, various models differ in the number of filaments that run the length of a fibril, and in the topological arrangement of these filaments. In addition to questions about the structure of Aβ40 monomers in fibrils, there are important unanswered questions about their structure in prefibrillar intermediates, which are of interest because they may represent the most neurotoxic form of Aβ40. To assess different models of fibril structure and to gain insight into the structure of prefibrillar intermediates, the relative solvent accessibility of amino acid residue side chains in fibrillar and prefibrillar Aβ40 preparations was characterized in solution by hydroxyl radical footprinting and structural mass spectrometry. A key to the application of this technology was the development of hydroxyl radical reactivity measures for individual side chains of Aβ40. Combined with mass-per-length measurements performed by dark-field electron microscopy, the results of this study are consistent with the core filament structure represented by two- and three-filament solid state nuclear magnetic resonance-based models of the Aβ40 fibril (such as 2LMN, 2LMO, 2LMP, and 2LMQ), with minor refinements, but they are inconsistent with the more recently proposed 2M4J model. The results also demonstrate that individual Aβ40 fibrils exhibit structural heterogeneity or polymorphism, where regions of two-filament structure alternate with regions of three-filament structure. The footprinting approach utilized in this study will be valuable for characterizing various fibrillar and nonfibrillar forms of the Aβ peptide.
format Online
Article
Text
id pubmed-4270378
institution National Center for Biotechnology Information
language English
publishDate 2014
publisher American Chemical Society
record_format MEDLINE/PubMed
spelling pubmed-42703782015-11-09 A Synchrotron-Based Hydroxyl Radical Footprinting Analysis of Amyloid Fibrils and Prefibrillar Intermediates with Residue-Specific Resolution Klinger, Alexandra L. Kiselar, Janna Ilchenko, Serguei Komatsu, Hiroaki Chance, Mark R. Axelsen, Paul H. Biochemistry [Image: see text] Structural models of the fibrils formed by the 40-residue amyloid-β (Aβ40) peptide in Alzheimer’s disease typically consist of linear polypeptide segments, oriented approximately perpendicular to the long axis of the fibril, and joined together as parallel in-register β-sheets to form filaments. However, various models differ in the number of filaments that run the length of a fibril, and in the topological arrangement of these filaments. In addition to questions about the structure of Aβ40 monomers in fibrils, there are important unanswered questions about their structure in prefibrillar intermediates, which are of interest because they may represent the most neurotoxic form of Aβ40. To assess different models of fibril structure and to gain insight into the structure of prefibrillar intermediates, the relative solvent accessibility of amino acid residue side chains in fibrillar and prefibrillar Aβ40 preparations was characterized in solution by hydroxyl radical footprinting and structural mass spectrometry. A key to the application of this technology was the development of hydroxyl radical reactivity measures for individual side chains of Aβ40. Combined with mass-per-length measurements performed by dark-field electron microscopy, the results of this study are consistent with the core filament structure represented by two- and three-filament solid state nuclear magnetic resonance-based models of the Aβ40 fibril (such as 2LMN, 2LMO, 2LMP, and 2LMQ), with minor refinements, but they are inconsistent with the more recently proposed 2M4J model. The results also demonstrate that individual Aβ40 fibrils exhibit structural heterogeneity or polymorphism, where regions of two-filament structure alternate with regions of three-filament structure. The footprinting approach utilized in this study will be valuable for characterizing various fibrillar and nonfibrillar forms of the Aβ peptide. American Chemical Society 2014-11-09 2014-12-16 /pmc/articles/PMC4270378/ /pubmed/25382225 http://dx.doi.org/10.1021/bi5010409 Text en Copyright © 2014 American Chemical Society This is an open access article published under an ACS AuthorChoice License (http://pubs.acs.org/page/policy/authorchoice_termsofuse.html) , which permits copying and redistribution of the article or any adaptations for non-commercial purposes.
spellingShingle Klinger, Alexandra L.
Kiselar, Janna
Ilchenko, Serguei
Komatsu, Hiroaki
Chance, Mark R.
Axelsen, Paul H.
A Synchrotron-Based Hydroxyl Radical Footprinting Analysis of Amyloid Fibrils and Prefibrillar Intermediates with Residue-Specific Resolution
title A Synchrotron-Based Hydroxyl Radical Footprinting Analysis of Amyloid Fibrils and Prefibrillar Intermediates with Residue-Specific Resolution
title_full A Synchrotron-Based Hydroxyl Radical Footprinting Analysis of Amyloid Fibrils and Prefibrillar Intermediates with Residue-Specific Resolution
title_fullStr A Synchrotron-Based Hydroxyl Radical Footprinting Analysis of Amyloid Fibrils and Prefibrillar Intermediates with Residue-Specific Resolution
title_full_unstemmed A Synchrotron-Based Hydroxyl Radical Footprinting Analysis of Amyloid Fibrils and Prefibrillar Intermediates with Residue-Specific Resolution
title_short A Synchrotron-Based Hydroxyl Radical Footprinting Analysis of Amyloid Fibrils and Prefibrillar Intermediates with Residue-Specific Resolution
title_sort synchrotron-based hydroxyl radical footprinting analysis of amyloid fibrils and prefibrillar intermediates with residue-specific resolution
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4270378/
https://www.ncbi.nlm.nih.gov/pubmed/25382225
http://dx.doi.org/10.1021/bi5010409
work_keys_str_mv AT klingeralexandral asynchrotronbasedhydroxylradicalfootprintinganalysisofamyloidfibrilsandprefibrillarintermediateswithresiduespecificresolution
AT kiselarjanna asynchrotronbasedhydroxylradicalfootprintinganalysisofamyloidfibrilsandprefibrillarintermediateswithresiduespecificresolution
AT ilchenkoserguei asynchrotronbasedhydroxylradicalfootprintinganalysisofamyloidfibrilsandprefibrillarintermediateswithresiduespecificresolution
AT komatsuhiroaki asynchrotronbasedhydroxylradicalfootprintinganalysisofamyloidfibrilsandprefibrillarintermediateswithresiduespecificresolution
AT chancemarkr asynchrotronbasedhydroxylradicalfootprintinganalysisofamyloidfibrilsandprefibrillarintermediateswithresiduespecificresolution
AT axelsenpaulh asynchrotronbasedhydroxylradicalfootprintinganalysisofamyloidfibrilsandprefibrillarintermediateswithresiduespecificresolution
AT klingeralexandral synchrotronbasedhydroxylradicalfootprintinganalysisofamyloidfibrilsandprefibrillarintermediateswithresiduespecificresolution
AT kiselarjanna synchrotronbasedhydroxylradicalfootprintinganalysisofamyloidfibrilsandprefibrillarintermediateswithresiduespecificresolution
AT ilchenkoserguei synchrotronbasedhydroxylradicalfootprintinganalysisofamyloidfibrilsandprefibrillarintermediateswithresiduespecificresolution
AT komatsuhiroaki synchrotronbasedhydroxylradicalfootprintinganalysisofamyloidfibrilsandprefibrillarintermediateswithresiduespecificresolution
AT chancemarkr synchrotronbasedhydroxylradicalfootprintinganalysisofamyloidfibrilsandprefibrillarintermediateswithresiduespecificresolution
AT axelsenpaulh synchrotronbasedhydroxylradicalfootprintinganalysisofamyloidfibrilsandprefibrillarintermediateswithresiduespecificresolution

Ejemplares similares