Atomic force microscopy reveals defects within mica supported lipid bilayers induced by the amyloidogenic human amylin peptide

J. D. Green; L. Kreplak; C. Goldsbury; X. Li Blatter; M. Stolz; G. S. Cooper; A. Seelig; J. Kistler; U. Aebi

doi:10.1016/j.jmb.2004.07.052

Atomic force microscopy reveals defects within mica supported lipid bilayers induced by the amyloidogenic human amylin peptide

J. D. Green, L. Kreplak, C. Goldsbury, X. Li Blatter, M. Stolz, G. S. Cooper, A. Seelig, J. Kistler, U. Aebi

Research output: Contribution to journal › Article › peer-review

148 Citations (Scopus)

Abstract

To date, over 20 peptides or proteins have been identified that can form amyloid fibrils in the body and are thought to cause disease. The mechanism by which amyloid peptides cause the cytotoxicity observed and disease is not understood. However, one of the major hypotheses is that amyloid peptides cause membrane perturbation. Hence, we have studied the interaction between lipid bilayers and the 37 amino acid residue polypeptide amylin, which is the primary constituent of the pancreatic amyloid associated with type 2 diabetes. Using a dye release assay we confirmed that the amyloidogenic human amylin peptide causes membrane disruption; however, time-lapse atomic force microscopy revealed that this did not occur by the formation of defined pores. On the contrary, the peptide induced the formation of small defects spreading over the lipid surface. We also found that rat amylin, which has 84% identity with human amylin but cannot form amyloid fibrils, could also induce similar lesions to supported lipid bilayers. The effect, however, for rat amylin but not human amylin, was inhibited under high ionic conditions. These data provide an alternative theory to pore formation, and how amyloid peptides may cause membrane disruption and possibly cytotoxicity.

Original language	English
Pages (from-to)	877-887
Number of pages	11
Journal	Journal of Molecular Biology
Volume	342
Issue number	3
DOIs	https://doi.org/10.1016/j.jmb.2004.07.052
Publication status	Published - Sept 17 2004
Externally published	Yes

Bibliographical note

Funding Information:
We thank Cynthia Tse, Stephanie Bailey and Liselotte Walti for administrative support. This work was supported by grants from the Swiss National Science Foundation (NCCR Nanoscale Science), Novartis Pharma, the M. E. Mueller Foundation of Switzerland, and the Canton Basel-Stadt. G.S.C. is supported by the Foundation for Research Science and Technology, and the Protemix Corporation.

ASJC Scopus Subject Areas

Biophysics
Structural Biology
Molecular Biology

PubMed: MeSH publication types

Journal Article
Research Support, Non-U.S. Gov't

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1016/j.jmb.2004.07.052

Cite this

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title = "Atomic force microscopy reveals defects within mica supported lipid bilayers induced by the amyloidogenic human amylin peptide",

abstract = "To date, over 20 peptides or proteins have been identified that can form amyloid fibrils in the body and are thought to cause disease. The mechanism by which amyloid peptides cause the cytotoxicity observed and disease is not understood. However, one of the major hypotheses is that amyloid peptides cause membrane perturbation. Hence, we have studied the interaction between lipid bilayers and the 37 amino acid residue polypeptide amylin, which is the primary constituent of the pancreatic amyloid associated with type 2 diabetes. Using a dye release assay we confirmed that the amyloidogenic human amylin peptide causes membrane disruption; however, time-lapse atomic force microscopy revealed that this did not occur by the formation of defined pores. On the contrary, the peptide induced the formation of small defects spreading over the lipid surface. We also found that rat amylin, which has 84% identity with human amylin but cannot form amyloid fibrils, could also induce similar lesions to supported lipid bilayers. The effect, however, for rat amylin but not human amylin, was inhibited under high ionic conditions. These data provide an alternative theory to pore formation, and how amyloid peptides may cause membrane disruption and possibly cytotoxicity.",

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note = "Funding Information: We thank Cynthia Tse, Stephanie Bailey and Liselotte Walti for administrative support. This work was supported by grants from the Swiss National Science Foundation (NCCR Nanoscale Science), Novartis Pharma, the M. E. Mueller Foundation of Switzerland, and the Canton Basel-Stadt. G.S.C. is supported by the Foundation for Research Science and Technology, and the Protemix Corporation.",

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AU - Seelig, A.

AU - Kistler, J.

AU - Aebi, U.

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N2 - To date, over 20 peptides or proteins have been identified that can form amyloid fibrils in the body and are thought to cause disease. The mechanism by which amyloid peptides cause the cytotoxicity observed and disease is not understood. However, one of the major hypotheses is that amyloid peptides cause membrane perturbation. Hence, we have studied the interaction between lipid bilayers and the 37 amino acid residue polypeptide amylin, which is the primary constituent of the pancreatic amyloid associated with type 2 diabetes. Using a dye release assay we confirmed that the amyloidogenic human amylin peptide causes membrane disruption; however, time-lapse atomic force microscopy revealed that this did not occur by the formation of defined pores. On the contrary, the peptide induced the formation of small defects spreading over the lipid surface. We also found that rat amylin, which has 84% identity with human amylin but cannot form amyloid fibrils, could also induce similar lesions to supported lipid bilayers. The effect, however, for rat amylin but not human amylin, was inhibited under high ionic conditions. These data provide an alternative theory to pore formation, and how amyloid peptides may cause membrane disruption and possibly cytotoxicity.

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Atomic force microscopy reveals defects within mica supported lipid bilayers induced by the amyloidogenic human amylin peptide

Abstract

Bibliographical note

ASJC Scopus Subject Areas

PubMed: MeSH publication types

UN SDGs

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