Stabilization and structural analysis of a membrane-associated hIAPP aggregation intermediate

Membrane-assisted amyloid formation is implicated in human diseases, and many of the aggregating species accelerate amyloid formation and induce cell death. While structures of membrane-associated intermediates would provide tremendous insights into the pathology and aid in the design of compounds t...

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Autores principales: Rodriguez Camargo, Diana C, Korshavn, Kyle J, Jussupow, Alexander, Raltchev, Kolio, Goricanec, David, Fleisch, Markus, Sarkar, Riddhiman, Xue, Kai, Aichler, Michaela, Mettenleiter, Gabriele, Walch, Axel Karl, Camilloni, Carlo, Hagn, Franz, Reif, Bernd, Ramamoorthy, Ayyalusamy
Formato: Online Artículo Texto
Lenguaje:English
Publicado: eLife Sciences Publications, Ltd 2017
Materias:
Biochemistry and Chemical Biology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5706959/
https://www.ncbi.nlm.nih.gov/pubmed/29148426
http://dx.doi.org/10.7554/eLife.31226
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author Rodriguez Camargo, Diana C
Korshavn, Kyle J
Jussupow, Alexander
Raltchev, Kolio
Goricanec, David
Fleisch, Markus
Sarkar, Riddhiman
Xue, Kai
Aichler, Michaela
Mettenleiter, Gabriele
Walch, Axel Karl
Camilloni, Carlo
Hagn, Franz
Reif, Bernd
Ramamoorthy, Ayyalusamy
author_facet Rodriguez Camargo, Diana C
Korshavn, Kyle J
Jussupow, Alexander
Raltchev, Kolio
Goricanec, David
Fleisch, Markus
Sarkar, Riddhiman
Xue, Kai
Aichler, Michaela
Mettenleiter, Gabriele
Walch, Axel Karl
Camilloni, Carlo
Hagn, Franz
Reif, Bernd
Ramamoorthy, Ayyalusamy
author_sort Rodriguez Camargo, Diana C
collection PubMed
description Membrane-assisted amyloid formation is implicated in human diseases, and many of the aggregating species accelerate amyloid formation and induce cell death. While structures of membrane-associated intermediates would provide tremendous insights into the pathology and aid in the design of compounds to potentially treat the diseases, it has not been feasible to overcome the challenges posed by the cell membrane. Here, we use NMR experimental constraints to solve the structure of a type-2 diabetes related human islet amyloid polypeptide intermediate stabilized in nanodiscs. ROSETTA and MD simulations resulted in a unique β-strand structure distinct from the conventional amyloid β-hairpin and revealed that the nucleating NFGAIL region remains flexible and accessible within this isolated intermediate, suggesting a mechanism by which membrane-associated aggregation may be propagated. The ability of nanodiscs to trap amyloid intermediates as demonstrated could become one of the most powerful approaches to dissect the complicated misfolding pathways of protein aggregation.
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spelling pubmed-57069592017-11-30 Stabilization and structural analysis of a membrane-associated hIAPP aggregation intermediate Rodriguez Camargo, Diana C Korshavn, Kyle J Jussupow, Alexander Raltchev, Kolio Goricanec, David Fleisch, Markus Sarkar, Riddhiman Xue, Kai Aichler, Michaela Mettenleiter, Gabriele Walch, Axel Karl Camilloni, Carlo Hagn, Franz Reif, Bernd Ramamoorthy, Ayyalusamy eLife Biochemistry and Chemical Biology Membrane-assisted amyloid formation is implicated in human diseases, and many of the aggregating species accelerate amyloid formation and induce cell death. While structures of membrane-associated intermediates would provide tremendous insights into the pathology and aid in the design of compounds to potentially treat the diseases, it has not been feasible to overcome the challenges posed by the cell membrane. Here, we use NMR experimental constraints to solve the structure of a type-2 diabetes related human islet amyloid polypeptide intermediate stabilized in nanodiscs. ROSETTA and MD simulations resulted in a unique β-strand structure distinct from the conventional amyloid β-hairpin and revealed that the nucleating NFGAIL region remains flexible and accessible within this isolated intermediate, suggesting a mechanism by which membrane-associated aggregation may be propagated. The ability of nanodiscs to trap amyloid intermediates as demonstrated could become one of the most powerful approaches to dissect the complicated misfolding pathways of protein aggregation. eLife Sciences Publications, Ltd 2017-11-17 /pmc/articles/PMC5706959/ /pubmed/29148426 http://dx.doi.org/10.7554/eLife.31226 Text en © 2017, Rodriguez Camargo et al http://creativecommons.org/licenses/by/4.0/ http://creativecommons.org/licenses/by/4.0/This article is distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use and redistribution provided that the original author and source are credited.
spellingShingle Biochemistry and Chemical Biology
Rodriguez Camargo, Diana C
Korshavn, Kyle J
Jussupow, Alexander
Raltchev, Kolio
Goricanec, David
Fleisch, Markus
Sarkar, Riddhiman
Xue, Kai
Aichler, Michaela
Mettenleiter, Gabriele
Walch, Axel Karl
Camilloni, Carlo
Hagn, Franz
Reif, Bernd
Ramamoorthy, Ayyalusamy
Stabilization and structural analysis of a membrane-associated hIAPP aggregation intermediate
title Stabilization and structural analysis of a membrane-associated hIAPP aggregation intermediate
title_full Stabilization and structural analysis of a membrane-associated hIAPP aggregation intermediate
title_fullStr Stabilization and structural analysis of a membrane-associated hIAPP aggregation intermediate
title_full_unstemmed Stabilization and structural analysis of a membrane-associated hIAPP aggregation intermediate
title_short Stabilization and structural analysis of a membrane-associated hIAPP aggregation intermediate
title_sort stabilization and structural analysis of a membrane-associated hiapp aggregation intermediate
topic Biochemistry and Chemical Biology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5706959/
https://www.ncbi.nlm.nih.gov/pubmed/29148426
http://dx.doi.org/10.7554/eLife.31226
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