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Investigation of supramolecular structures in various aqueous solutions of an amyloid forming peptide using small-angle X-ray scattering
Uppsala University, Disciplinary Domain of Medicine and Pharmacy, Faculty of Pharmacy, Department of Medicinal Chemistry. (Farmaceutisk fysikalisk kemi)ORCID iD: 0009-0002-2561-1513
AstraZeneca, Adv Drug Delivery, Pharmaceut Sci, R&D, S-43183 Gothenburg, Sweden..
Uppsala University, Disciplinary Domain of Science and Technology, Chemistry, Department of Chemistry - Ångström, Physical Chemistry.ORCID iD: 0000-0002-3746-6811
Uppsala University, Disciplinary Domain of Science and Technology, Chemistry, Department of Chemistry - Ångström, Physical Chemistry.ORCID iD: 0000-0003-0674-2219
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2024 (English)In: Soft Matter, ISSN 1744-683X, E-ISSN 1744-6848, Vol. 20, no 10, p. 2272-2279Article in journal (Refereed) Published
Abstract [en]

Aggregation of peptide molecules into amyloid fibrils is a characteristic feature of several degenerative diseases. However, the details behind amyloid-formation, and other self-assembled peptide aggregates, remain poorly understood. In this study, we have used small-angle X-ray scattering (SAXS), static and dynamic light scattering (SLS and DLS) as well as cryogenic transmission electron microscopy (cryo-TEM) to determine the structural geometry of self-assembled peptide aggregates in various dilute aqueous solutions. Pramlintide was used as a model peptide to assess the aggregation behaviour of an amyloid-forming peptide. The effects of adding sodium chloride (NaCl), sodium thiocyanate (NaSCN), and sodium fluoride (NaF) and the co-solvent dimethyl sulfoxide (DMSO) on the aggregation behaviour were studied. Our scattering data analysis demonstrates that small oligomeric fibrils aggregate to form networks of supramolecular assemblies with fractal dimensions. The choice of anion in small amounts of added salt has a significant impact on the size of the fibrils as well as on the fractal dimensions of supramolecular clusters. In DMSO the fractal dimension decreased with increasing DMSO concentration, indicating the formation of a less compact structure of the supramolecular assemblies. The peptide pramlintide forms oligomeric species in solution, which make up a supramolecular network characterised by fractal dimensions. The fractal dimension of the network depends on solvent additive.
Place, publisher, year, edition, pages
Royal Society of Chemistry, 2024. Vol. 20, no 10, p. 2272-2279
National Category
Physical Chemistry Biochemistry Molecular Biology
Identifiers
URN: urn:nbn:se:uu:diva-528361DOI: 10.1039/d3sm01172kISI: 001161006900001PubMedID: 38353286OAI: oai:DiVA.org:uu-528361DiVA, id: diva2:1859435
Part of project
The Swedish Drug Delivery Center (SweDeliver), Vinnova
Funder
Vinnova, 2019-00048Available from: 2024-05-21 Created: 2024-05-21 Last updated: 2025-12-09Bibliographically approved
In thesis
1. Self-assembly of therapeutic peptides
Open this publication in new window or tab >>Self-assembly of therapeutic peptides
2026 (English)Doctoral thesis, comprehensive summary (Other academic)
Abstract [en]

Peptides as therapeutic agents have gained significant interest during the last few decades due to their specificity, potency, and efficacy compared with small-molecular drugs. However, peptide aggregation remains a considerable concern during production, formulation, and storage of therapeutic peptides. Peptide aggregation can result in loss of therapeutic effect or, in worst case, immunogenic response and side effects. However, in some cases, peptide aggregation can be utilised to achieve extended-release formulations. In both scenarios, the aggregation mechanisms are essential to understand in order to predict and prevent aggregation, or know when aggregation can be utilised. Excipients in peptide formulations and biological components can also affect the aggregation behaviour of therapeutic peptides, highlighting the need to investigate the effect of additional components on peptide self-assembly. 

The structure of self-assembled peptide aggregates can offer insights into the aggregation mechanisms of therapeutic peptides. The size and structure of peptide self-assemblies can be investigated with scattering techniques, such as small-angle X-ray and neutron scattering and dynamic and static light scattering. 

The aggregation behaviour of three different peptides were investigated based on structural determination of peptide aggregates with scattering techniques. The peptides were dissolved in aqueous solutions and additional components were added gradually to investigate the specific effects of added salt, varying pH, different buffers, and amphiphilic compounds on peptide aggregate structure. Small-angle scattering data were analysed by model fitting to determine the size and structure of self-assembled aggregates. 

The different peptides investigated in this thesis displayed different aggregation behaviour in solution and different interaction behaviour with added components, highlighting the wide variety of possible aggregate structures peptides can form in solution. The supramolecular network formed by an amyloid-forming peptide, the type of interaction behaviour of a small cyclical peptide with a surfactant, and the ability of a lipidated peptide to dissolve phospholipids could be studied through combining different scattering techniques. Using systems with few components, the work in this thesis provides strategies to explore the fundamentals of therapeutic peptide aggregation which can be useful during design and formulation of therapeutic peptides, as well as understanding the behaviour of a peptide drug after administration. 
Place, publisher, year, edition, pages
Uppsala: Acta Universitatis Upsaliensis, 2026. p. 59
Series
Digital Comprehensive Summaries of Uppsala Dissertations from the Faculty of Pharmacy, ISSN 1651-6192 ; 394
Keywords
Peptides, aggregation, self-assembly, SAXS, SANS, micelles, drug delivery, peptide formulations
National Category
Physical Chemistry
Research subject
Pharmaceutical Science
Identifiers
urn:nbn:se:uu:diva-572871 (URN)978-91-513-2705-1 (ISBN)
Public defence
2026-02-11, A1:111a, Husargatan 3, Uppsala, 09:00 (English)
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Supervisors
Available from: 2026-01-20 Created: 2025-12-09 Last updated: 2026-02-10

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Brunzell, EllenGedda, LarsEdwards, KatarinaBergström, L. Magnus

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