Dimerization of the Full-Length Alzheimer Amyloid β-Peptide (Aβ42) in Explicit Aqueous Solution: A Molecular Dynamics Study

Zhu, Xiaoxia; Bora, Ram Prasad; Barman, Arghya; Singh, Rajiv R. P.; Prabhakar, Rajeev

doi:10.1021/jp210019h

Cited by 53 publications

(81 citation statements)

References 118 publications

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“…This is due to stabilization provide by several hydrogen bonds and hydrophobic interactions between the CHC regions of the monomers. These results are in line with the results of MD simulation of Ab 42 dimerization by Prabhakar and co-workers [47].…”

Section: The Effect Of P7c3 On Ab Peptide Aggregationsupporting

confidence: 92%

“…The mechanism of dimerization of the full-length Ab 42 peptides and structural properties of the three most stable dimers through ''bottom up'' all-atom MD simulations in aqueous solution was performed by Prabhakar and coworkers [47]. In the bottom up approach the dimerization process starts from the native structures of the monomers.…”

Section: The Effect Of P7c3 On Ab Peptide Aggregationmentioning

confidence: 99%

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The binding of small carbazole derivative (P7C3) to protofibrils of the Alzheimer’s disease and β-secretase: Molecular dynamics simulation studies

et al. 2015

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Section: The Effect Of P7c3 On Ab Peptide Aggregationsupporting

confidence: 92%

Section: The Effect Of P7c3 On Ab Peptide Aggregationmentioning

confidence: 99%

The binding of small carbazole derivative (P7C3) to protofibrils of the Alzheimer’s disease and β-secretase: Molecular dynamics simulation studies

et al. 2015

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“…For example in different conditions, Aβ can aggregate in the form of monomers to oligos and finally in cytotoxic protofilaments of Aβ 1–42. In addition, there are studies that show the specific amino acid regions that favor the β-sheet assembly into insoluble protofilaments, in order to correlate these results with those obtained with NMR and X-ray diffraction experiments (Buchete et al, 2005; Zhu et al, 2012; Lee et al, 2016). However, neither the molecular mechanism nor the different structural conformations that Aβ 1–42 adopts, from the monomer phase to its final aggregation in insoluble protofibrils, have been established in animal models.…”

Section: Introductionmentioning

confidence: 99%

Structural Changes of Amyloid Beta in Hippocampus of Rats Exposed to Ozone: A Raman Spectroscopy Study

Rivas‐Arancibia

Rodrı́guez-Martı́nez

Badillo‐Ramírez

et al. 2017

Front. Mol. Neurosci.

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The aim of this work was to study the effect of oxidative stress on the structural changes of the secondary peptide structure of amyloid beta 1–42 (Aβ 1–42), in the dentate gyrus of hippocampus of rats exposed to low doses of ozone. The animals were exposed to ozone-free air (control group) and 0.25 ppm ozone during 7, 15, 30, 60, and 90 days, respectively. The samples were studied by: (1) Raman spectroscopy to detect the global conformational changes in peptides with α-helix and β-sheet secondary structure, following the deconvolution profile of the amide I band; and (2) immunohistochemistry against Aβ 1–42. The results of the deconvolutions of the amide I band indicate that, ozone exposure causes a progressively decrease in the abundance percentage of α-helix secondary structure. Furthermore, the β-sheet secondary structure increases its abundance percentage. After 60 days of ozone exposure, the β-sheet band is identified in a similar wavenumber of the Aβ 1–42 peptide standard. Immunohistochemistry assays show an increase of Aβ 1–42 immunoreactivity, coinciding with the conformational changes observed in the Raman spectroscopy of Aβ 1–42 at 60 and 90 days. In conclusion, oxidative stress produces changes in the folding process of amyloid beta peptide structure in the dentate gyrus, leading to its conformational change in a final β-sheet structure. This is associated to an increase in Aβ 1–42 expression, similar to the one that happens in the brain of Alzheimer’s Disease (AD) patients.

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“…Even with the sophistication of modern techniques, experimental characterization of the monomeric Ab peptides remains challenging due to the intrinsically disordered and rapidly interchanging nature of the system. On the other hand, molecular dynamics (MD) simulations at different resolutions have been widely used to complement experiments (45) in providing detailed information on the structure of various Ab species ranging from monomers (23,(46)(47)(48)(49)(50) to oligomers (51,52) to protofibrils (53) to fibrils (54). Interactions of different Ab species with toxicity and aggregation inhibitors (55)(56)(57) and with lipid bilayers (58,59) also have been studied using MD.…”

Section: Introductionmentioning

confidence: 99%

Alzheimer’s Protective A2T Mutation Changes the Conformational Landscape of the Aβ1–42 Monomer Differently Than Does the A2V Mutation

Das

Murray

Belfort

2015

Biophysical Journal

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The aggregation of amyloid-β (Aβ) peptides plays a crucial role in the etiology of Alzheimer's disease (AD). Recently, it has been reported that an A2T mutation in Aβ can protect against AD. Interestingly, a nonpolar A2V mutation also has been found to offer protection against AD in the heterozygous state, although it causes early-onset AD in homozygous carriers. Since the conformational landscape of the Aβ monomer is known to directly contribute to the early-stage aggregation mechanism, it is important to characterize the effects of the A2T and A2V mutations on Aβ₁₋₄₂ monomer structure. Here, we have performed extensive atomistic replica-exchange molecular dynamics simulations of the solvated wild-type (WT), A2V, and A2T Aβ₁₋₄₂ monomers. Our simulations reveal that although all three variants remain as collapsed coils in solution, there exist significant structural differences among them at shorter timescales. A2V exhibits an enhanced double-hairpin population in comparison to the WT, similar to those reported in toxic WT Aβ₁₋₄₂ oligomers. Such double-hairpin formation is caused by hydrophobic clustering between the N-terminus and the central and C-terminal hydrophobic patches. In contrast, the A2T mutation causes the N-terminus to engage in unusual electrostatic interactions with distant residues, such as K16 and E22, resulting in a unique population comprising only the C-terminal hairpin. These findings imply that a single A2X (where X = V or T) mutation in the primarily disordered N-terminus of the Aβ₁₋₄₂ monomer can dramatically alter the β-hairpin population and switch the equilibrium toward alternative structures. The atomistically detailed, comparative view of the structural landscapes of A2V and A2T variant monomers obtained in this study can enhance our understanding of the mechanistic differences in their early-stage aggregation.

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Dimerization of the Full-Length Alzheimer Amyloid β-Peptide (Aβ42) in Explicit Aqueous Solution: A Molecular Dynamics Study

Cited by 53 publications

References 118 publications

The binding of small carbazole derivative (P7C3) to protofibrils of the Alzheimer’s disease and β-secretase: Molecular dynamics simulation studies

The binding of small carbazole derivative (P7C3) to protofibrils of the Alzheimer’s disease and β-secretase: Molecular dynamics simulation studies

Structural Changes of Amyloid Beta in Hippocampus of Rats Exposed to Ozone: A Raman Spectroscopy Study

Alzheimer’s Protective A2T Mutation Changes the Conformational Landscape of the Aβ1–42 Monomer Differently Than Does the A2V Mutation

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