Lipid Modulation in the Formation of β-Sheet Structures. Implications for De Novo Design of Human Islet Amyloid Polypeptide and the Impact on β-Cell Homeostasis

Human islet amyloid polypeptide (hIAPP) corresponds to a 37-residue hormone present in insulin granules that maintains a high propensity to form β-sheet structures during co-secretion with insulin. Previously, employing a biomimetic approach, we proposed a panel of optimized IAPP sequences with only...

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Autores principales: Martínez-Navarro, Israel, Díaz-Molina, Raúl, Pulido-Capiz, Angel, Mas-Oliva, Jaime, Luna-Reyes, Ismael, Rodríguez-Velázquez, Eustolia, Rivero, Ignacio A., Ramos-Ibarra, Marco A., Alatorre-Meda, Manuel, García-González, Victor
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2020
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7563882/
https://www.ncbi.nlm.nih.gov/pubmed/32824918
http://dx.doi.org/10.3390/biom10091201
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author Martínez-Navarro, Israel
Díaz-Molina, Raúl
Pulido-Capiz, Angel
Mas-Oliva, Jaime
Luna-Reyes, Ismael
Rodríguez-Velázquez, Eustolia
Rivero, Ignacio A.
Ramos-Ibarra, Marco A.
Alatorre-Meda, Manuel
García-González, Victor
author_facet Martínez-Navarro, Israel
Díaz-Molina, Raúl
Pulido-Capiz, Angel
Mas-Oliva, Jaime
Luna-Reyes, Ismael
Rodríguez-Velázquez, Eustolia
Rivero, Ignacio A.
Ramos-Ibarra, Marco A.
Alatorre-Meda, Manuel
García-González, Victor
author_sort Martínez-Navarro, Israel
collection PubMed
description Human islet amyloid polypeptide (hIAPP) corresponds to a 37-residue hormone present in insulin granules that maintains a high propensity to form β-sheet structures during co-secretion with insulin. Previously, employing a biomimetic approach, we proposed a panel of optimized IAPP sequences with only one residue substitution that shows the capability to reduce amyloidogenesis. Taking into account that specific membrane lipids have been considered as a key factor in the induction of cytotoxicity, in this study, following the same design strategy, we characterize the effect of a series of lipids upon several polypeptide domains that show the highest aggregation propensity. The characterization of the C-native segment of hIAPP (residues F(23)-Y(37)), together with novel variants F(23)R and I(26)A allowed us to demonstrate an effect upon the formation of β-sheet structures. Our results suggest that zwitterionic phospholipids promote adsorption of the C-native segments at the lipid-interface and β-sheet formation with the exception of the F(23)R variant. Moreover, the presence of cholesterol did not modify this behavior, and the β-sheet structural transitions were not registered when the N-terminal domain of hIAPP (K(1)-S(20)) was characterized. Considering that insulin granules are enriched in phosphatidylserine (PS), the property of lipid vesicles containing negatively charged lipids was also evaluated. We found that these types of lipids promote β-sheet conformational transitions in both the C-native segment and the new variants. Furthermore, these PS/peptides arrangements are internalized in Langerhans islet β-cells, localized in the endoplasmic reticulum, and trigger critical pathways such as unfolded protein response (UPR), affecting insulin secretion. Since this phenomenon was associated with the presence of cytotoxicity on Langerhans islet β-cells, it can be concluded that the anionic lipid environment and degree of solvation are critical conditions for the stability of segments with the propensity to form β-sheet structures, a situation that will eventually affect the structural characteristics and stability of IAPP within insulin granules, thus modifying the insulin secretion.
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spelling pubmed-75638822020-10-27 Lipid Modulation in the Formation of β-Sheet Structures. Implications for De Novo Design of Human Islet Amyloid Polypeptide and the Impact on β-Cell Homeostasis Martínez-Navarro, Israel Díaz-Molina, Raúl Pulido-Capiz, Angel Mas-Oliva, Jaime Luna-Reyes, Ismael Rodríguez-Velázquez, Eustolia Rivero, Ignacio A. Ramos-Ibarra, Marco A. Alatorre-Meda, Manuel García-González, Victor Biomolecules Article Human islet amyloid polypeptide (hIAPP) corresponds to a 37-residue hormone present in insulin granules that maintains a high propensity to form β-sheet structures during co-secretion with insulin. Previously, employing a biomimetic approach, we proposed a panel of optimized IAPP sequences with only one residue substitution that shows the capability to reduce amyloidogenesis. Taking into account that specific membrane lipids have been considered as a key factor in the induction of cytotoxicity, in this study, following the same design strategy, we characterize the effect of a series of lipids upon several polypeptide domains that show the highest aggregation propensity. The characterization of the C-native segment of hIAPP (residues F(23)-Y(37)), together with novel variants F(23)R and I(26)A allowed us to demonstrate an effect upon the formation of β-sheet structures. Our results suggest that zwitterionic phospholipids promote adsorption of the C-native segments at the lipid-interface and β-sheet formation with the exception of the F(23)R variant. Moreover, the presence of cholesterol did not modify this behavior, and the β-sheet structural transitions were not registered when the N-terminal domain of hIAPP (K(1)-S(20)) was characterized. Considering that insulin granules are enriched in phosphatidylserine (PS), the property of lipid vesicles containing negatively charged lipids was also evaluated. We found that these types of lipids promote β-sheet conformational transitions in both the C-native segment and the new variants. Furthermore, these PS/peptides arrangements are internalized in Langerhans islet β-cells, localized in the endoplasmic reticulum, and trigger critical pathways such as unfolded protein response (UPR), affecting insulin secretion. Since this phenomenon was associated with the presence of cytotoxicity on Langerhans islet β-cells, it can be concluded that the anionic lipid environment and degree of solvation are critical conditions for the stability of segments with the propensity to form β-sheet structures, a situation that will eventually affect the structural characteristics and stability of IAPP within insulin granules, thus modifying the insulin secretion. MDPI 2020-08-19 /pmc/articles/PMC7563882/ /pubmed/32824918 http://dx.doi.org/10.3390/biom10091201 Text en © 2020 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Martínez-Navarro, Israel
Díaz-Molina, Raúl
Pulido-Capiz, Angel
Mas-Oliva, Jaime
Luna-Reyes, Ismael
Rodríguez-Velázquez, Eustolia
Rivero, Ignacio A.
Ramos-Ibarra, Marco A.
Alatorre-Meda, Manuel
García-González, Victor
Lipid Modulation in the Formation of β-Sheet Structures. Implications for De Novo Design of Human Islet Amyloid Polypeptide and the Impact on β-Cell Homeostasis
title Lipid Modulation in the Formation of β-Sheet Structures. Implications for De Novo Design of Human Islet Amyloid Polypeptide and the Impact on β-Cell Homeostasis
title_full Lipid Modulation in the Formation of β-Sheet Structures. Implications for De Novo Design of Human Islet Amyloid Polypeptide and the Impact on β-Cell Homeostasis
title_fullStr Lipid Modulation in the Formation of β-Sheet Structures. Implications for De Novo Design of Human Islet Amyloid Polypeptide and the Impact on β-Cell Homeostasis
title_full_unstemmed Lipid Modulation in the Formation of β-Sheet Structures. Implications for De Novo Design of Human Islet Amyloid Polypeptide and the Impact on β-Cell Homeostasis
title_short Lipid Modulation in the Formation of β-Sheet Structures. Implications for De Novo Design of Human Islet Amyloid Polypeptide and the Impact on β-Cell Homeostasis
title_sort lipid modulation in the formation of β-sheet structures. implications for de novo design of human islet amyloid polypeptide and the impact on β-cell homeostasis
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7563882/
https://www.ncbi.nlm.nih.gov/pubmed/32824918
http://dx.doi.org/10.3390/biom10091201
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