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Amyloid beta-peptides 1-40 and 1-42 form oligomers with mixed beta-sheets
Stockholms universitet, Naturvetenskapliga fakulteten, Institutionen för biokemi och biofysik.
Stockholms universitet, Naturvetenskapliga fakulteten, Institutionen för biokemi och biofysik.ORCID-id: 0000-0003-1399-748X
ORCID-id: 0000-0001-5886-2023
Stockholms universitet, Naturvetenskapliga fakulteten, Institutionen för biokemi och biofysik.ORCID-id: 0000-0001-5784-7673
Rekke forfattare: 42017 (engelsk)Inngår i: Chemical Science, ISSN 2041-6520, E-ISSN 2041-6539, Vol. 8, nr 12, s. 8247-8254Artikkel i tidsskrift (Fagfellevurdert) Published
Abstract [en]

Two main amyloid-beta peptides of different length (A beta(40) and A beta(42)) are involved in Alzheimer's disease. Their relative abundance is decisive for the severity of the disease and mixed oligomers may contribute to the toxic species. However, little is know about the extent of mixing. To study whether A beta(40) and A beta(42) co-aggregate, we used Fourier transform infrared spectroscopy in combination with C-13-labeling and spectrum calculation and focused on the amide I vibration, which is sensitive to backbone structure. Mixtures of monomeric labeled A beta(40) and unlabeled A beta(42) (and vice versa) were co-incubated for similar to 20 min and their infrared spectrum recorded. The position of the main C-13-amide I' band shifted to higher wavenumbers with increasing admixture of C-12-peptide due to the presence of C-12-amides in the vicinity of C-13-amides. The results indicate that A beta(40) and A beta(42) form mixed oligomers with a largely random distribution of A beta(40) and A beta(42) strands in their beta-sheets. The structures of the mixed oligomers are intermediate between those of the pure oligomers. There is no indication that one of the peptides forces the backbone structure of its oligomers on the other peptide when they are mixed as monomers. We also demonstrate that isotope-edited infrared spectroscopy can distinguish aggregation modulators that integrate into the backbone structure of their interaction partner from those that do not. As an example for the latter case, the pro-inflammatory calcium binding protein S100A9 is shown not to incorporate into the b-sheets of A beta(42).
sted, utgiver, år, opplag, sider
2017. Vol. 8, nr 12, s. 8247-8254
HSV kategori
Forskningsprogram
biofysik
Identifikatorer
URN: urn:nbn:se:su:diva-150050DOI: 10.1039/c7sc01743jISI: 000415877000043OAI: oai:DiVA.org:su-150050DiVA, id: diva2:1166016
Tilgjengelig fra: 2017-12-14 Laget: 2017-12-14 Sist oppdatert: 2022-03-23bibliografisk kontrollert
Inngår i avhandling
1. Computational infrared spectroscopy: Calculation of the amide I absorption of proteins
Åpne denne publikasjonen i ny fane eller vindu >>Computational infrared spectroscopy: Calculation of the amide I absorption of proteins
2020 (engelsk)Doktoravhandling, med artikler (Annet vitenskapelig)
Abstract [en]

Infrared spectroscopy is an important technique that allows to retrieve structural information from the analysis of absorption spectra. The main application of infrared spectroscopy within life science is the study of the amide I band, which is correlated with protein backbone conformation and, consequently, with the secondary structure of proteins. However, band assignment and interpretation of the infrared spectra is not straightforward.

Therefore, several simulation methods were developed to guide the interpretation of experimental amide I spectra. In this thesis, one of these methods is a normal mode analysis, which is based on the evaluation of the intrinsic vibration of the amide groups and the interactions between them. The calculation considers several effects: transition dipole coupling, nearest neighbor interaction, the local environment effect and the effect of hydrogen bond. From the normal mode analysis, it is possible to obtain the simulated infrared spectrum and the contribution of each amide group to a specific spectral range of the spectrum.

The aim of this thesis and of the included publications is to explain this approach, to improve it and to show its potential. Results from simulations were compared with experimental data for different proteins of interest: amyloid-β oligomers and β-helix proteins. Simulated and experimental infrared spectra showed similar bands. Simulations also provided additional conclusions: they confirmed the random mixing of amyloid-β peptides in oligomers; they suggested that amyloid-β peptides contribute at least two strands in the structure of the oligomers; they revealed that the high wavenumber band, typical of antiparallel β-sheets, can be caused by other secondary structures, but not by parallel β-sheets. In addition, to verify and to improve the accuracy of this approach, simulation results were also put in a direct comparison with results from density functional theory calculations. From this comparison, a new optimal set of parameters for the calculations is suggested.
sted, utgiver, år, opplag, sider
Stockholm: Department of Biochemistry and Biophysics, Stockholm University, 2020. s. 63
Emneord
infrared spectroscopy, FTIR, simulation, calculation, amide I, transition dipole coupling, F matrix, protein, amyloid β, oligomers, β-helix
HSV kategori
Forskningsprogram
biofysik
Identifikatorer
urn:nbn:se:su:diva-179912 (URN)978-91-7911-074-1 (ISBN)978-91-7911-075-8 (ISBN)
Disputas
2020-04-29, Magnélisalen, Kemiska övningslaboratoriet, Svante Arrhenius väg 16B, Stockholm, 10:00 (engelsk)
Opponent
Veileder
Merknad

At the time of the doctoral defense, the following paper was unpublished and had a status as follows: Paper 4: Manuscript.

Tilgjengelig fra: 2020-04-06 Laget: 2020-03-13 Sist oppdatert: 2022-02-26bibliografisk kontrollert

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Baldassarre, MaurizioBaronio, Cesare M.Morozova-Roche, Ludmilla A.Barth, Andreas

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