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Literature DB >> 23642026

Molecular mechanism of misfolding and aggregation of Aβ(13-23).

Sándor Lovas¹, Yuliang Zhang, Junping Yu, Yuri L Lyubchenko.

Abstract

The misfolding and self-assembly of the amyloid-beta (Aβ) peptide into aggregates is a molecular signature of the development of Alzheimer's disease, but molecular mechanisms of the peptide aggregation remain unknown. Here, we combined Atomic Force Microscopy (AFM) and Molecular Dynamics (MD) simulations to characterize the misfolding process of an Aβ peptide. Dynamic force spectroscopy AFM analysis showed that the peptide forms stable dimers with a lifetime of ∼1 s. During MD simulations, isolated monomers gradually adopt essentially similar nonstructured conformations independent from the initial structure. However, when two monomers approach their structure changes dramatically, and the conformational space for the two monomers become restricted. The arrangement of monomers in antiparallel orientation leads to the cooperative formation of β-sheet conformation. Interactions, including hydrogen bonds, salt bridges, and weakly polar interactions of side chains stabilize the structure of the dimer. Under the applied force, the dimer, as during the AFM experiments, dissociates in a cooperative manner. Thus, misfolding of the Aβ peptide proceeds via the loss of conformational flexibility and formation of stable dimers suggesting their key role in the subsequent Aβ aggregation process.

Entities: Chemical Disease Gene Mutation Species

Mesh：

Substances：
Amyloid beta-Peptides

Year: 2013 PMID： 23642026 PMCID： PMC3695694 DOI： 10.1021/jp402938p

Source DB: PubMed Journal: J Phys Chem B ISSN： 1520-5207 Impact factor: 2.991

62 in total

1. The Protein Data Bank.

Authors: H M Berman; J Westbrook; Z Feng; G Gilliland; T N Bhat; H Weissig; I N Shindyalov; P E Bourne
Journal: Nucleic Acids Res Date: 2000-01-01 Impact factor: 16.971

2. Protein interactions and misfolding analyzed by AFM force spectroscopy.

Authors: Chad McAllister; Mikhail A Karymov; Yoshiko Kawano; Alexander Y Lushnikov; Andrew Mikheikin; Vladimir N Uversky; Yuri L Lyubchenko
Journal: J Mol Biol Date: 2005-11-02 Impact factor: 5.469

3. Molecular alignment within beta-sheets in Abeta(14-23) fibrils: solid-state NMR experiments and theoretical predictions.

Authors: Zimei Bu; Yuan Shi; David J E Callaway; Robert Tycko
Journal: Biophys J Date: 2006-10-20 Impact factor: 4.033

4. Atomic-level description of amyloid beta-dimer formation.

Authors: S Gnanakaran; Ruth Nussinov; Angel E García
Journal: J Am Chem Soc Date: 2006-02-22 Impact factor: 15.419

Review 5. Fluorescence as a method to reveal structures and membrane-interactions of amyloidogenic proteins.

Authors: Larissa A Munishkina; Anthony L Fink
Journal: Biochim Biophys Acta Date: 2007-03-28

6. Calculation of weakly polar interaction energies in polypeptides using density functional and local Møller-Plesset perturbation theory.

Authors: József Csontos; Nicholas Y Palermo; Richard F Murphy; Sándor Lovas
Journal: J Comput Chem Date: 2008-06 Impact factor: 3.376

7. Amyloid-β protein oligomerization and the importance of tetramers and dodecamers in the aetiology of Alzheimer's disease.

Authors: Summer L Bernstein; Nicholas F Dupuis; Noel D Lazo; Thomas Wyttenbach; Margaret M Condron; Gal Bitan; David B Teplow; Joan-Emma Shea; Brandon T Ruotolo; Carol V Robinson; Michael T Bowers
Journal: Nat Chem Date: 2009-07 Impact factor: 24.427

8. Amyloid fibril formation by A beta 16-22, a seven-residue fragment of the Alzheimer's beta-amyloid peptide, and structural characterization by solid state NMR.

Authors: J J Balbach; Y Ishii; O N Antzutkin; R D Leapman; N W Rizzo; F Dyda; J Reed; R Tycko
Journal: Biochemistry Date: 2000-11-14 Impact factor: 3.162

9. Supramolecular structure in full-length Alzheimer's beta-amyloid fibrils: evidence for a parallel beta-sheet organization from solid-state nuclear magnetic resonance.

Authors: John J Balbach; Aneta T Petkova; Nathan A Oyler; Oleg N Antzutkin; David J Gordon; Stephen C Meredith; Robert Tycko
Journal: Biophys J Date: 2002-08 Impact factor: 4.033

Molecular mechanism of misfolding and aggregation of Aβ(13-23).

1. The Protein Data Bank.

2. Protein interactions and misfolding analyzed by AFM force spectroscopy.

3. Molecular alignment within beta-sheets in Abeta(14-23) fibrils: solid-state NMR experiments and theoretical predictions.

4. Atomic-level description of amyloid beta-dimer formation.

Review 5. Fluorescence as a method to reveal structures and membrane-interactions of amyloidogenic proteins.

6. Calculation of weakly polar interaction energies in polypeptides using density functional and local Møller-Plesset perturbation theory.

7. Amyloid-β protein oligomerization and the importance of tetramers and dodecamers in the aetiology of Alzheimer's disease.

8. Amyloid fibril formation by A beta 16-22, a seven-residue fragment of the Alzheimer's beta-amyloid peptide, and structural characterization by solid state NMR.

9. Supramolecular structure in full-length Alzheimer's beta-amyloid fibrils: evidence for a parallel beta-sheet organization from solid-state nuclear magnetic resonance.

10. Role of small oligomers on the amyloidogenic aggregation free-energy landscape.

1. Direct Detection of α-Synuclein Dimerization Dynamics: Single-Molecule Fluorescence Analysis.

2. The structure of misfolded amyloidogenic dimers: computational analysis of force spectroscopy data.

3. A flexible nanoarray approach for the assembly and probing of molecular complexes.

4. Single-molecule probing of amyloid nano-ensembles using the polymer nanoarray approach.

5. Piecewise All-Atom SMD Simulations Reveal Key Secondary Structures in Luciferase Unfolding Pathway.

6. Probing the Basis of α-Synuclein Aggregation by Comparing Simulations to Single-Molecule Experiments.

7. Probing Intermolecular Interactions within the Amyloid β Trimer Using a Tethered Polymer Nanoarray.

8. A Metal-free Click Chemistry Approach for the Assembly and Probing of Biomolecules.

9. Probing of Amyloid Aβ (14-23) Trimers by Single-Molecule Force Spectroscopy.

10. Nanoscale Dynamics of Amyloid β-42 Oligomers As Revealed by High-Speed Atomic Force Microscopy.