Distinct Effects of Zn2+, Cu2+, Fe3+, and Al3+ on Amyloid-β Stability, Oligomerization, and Aggregation

Chen, Wei Ting; Liao, Yi Hung; Yu, Hsiao-Wei; Cheng, Irene H.; Chen, Yun‐Ru

doi:10.1074/jbc.m110.177246

Cited by 180 publications

(163 citation statements)

References 73 publications

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“…This indicates that the remaining soluble peptide was already fully loaded with Cu(II), and that the aggregation of a soluble A␤-Cu y complex is rate-limiting as observed under equimolar conditions. Recently it has been shown that Cu(II) decreases the hydrophobic exposed protein surfaces of A␤ when added in supraequimolar ratios (43), which may explain the observed increased solubility of the A␤-Cu complex.…”

Section: Cu(ii):a␤ 1-40 Ratiomentioning

confidence: 99%

Cu(II) Mediates Kinetically Distinct, Non-amyloidogenic Aggregation of Amyloid-β Peptides

Pedersen

Østergaard

Rozlosnik

et al. 2011

Journal of Biological Chemistry

118

160

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Cu(II) ions are implicated in the pathogenesis of Alzheimer disease by influencing the aggregation of the amyloid-␤ (A␤)peptide. Elucidating the underlying Cu(II)-induced A␤ aggregation is paramount for understanding the role of Cu(II) in the pathology of Alzheimer disease. The aim of this study was to characterize the qualitative and quantitative influence of Cu(II) on the extracellular aggregation mechanism and aggregate morphology of A␤ 1-40 using spectroscopic, microelectrophoretic, mass spectrometric, and ultrastructural techniques. We found that the Cu(II):A␤ ratio in solution has a major influence on (i) the aggregation kinetics/mechanism of A␤, because three different kinetic scenarios were observed depending on the Cu(II):A␤ ratio, (ii) the metal:peptide stoichiometry in the aggregates, which increased to 1.4 at supra-equimolar Cu(II):A␤ ratio; and (iii) the morphology of the aggregates, which shifted from fibrillar to non-fibrillar at increasing Cu(II):A␤ ratios. We observed dynamic morphological changes of the aggregates, and that the formation of spherical aggregates appeared to be a common morphological end point independent on the Cu(II) concentration. Experiments with A␤ 1-42 were compatible with the conclusions for A␤ 1-40 even though the low solubility of A␤ 1-42 precluded examination under the same conditions as for the A␤ 1-40 . Experiments with A␤ 1-16 and A␤ 1-28 showed that other parts than the Cu(II)-binding His residues were important for Cu(II)-induced A␤ aggregation. Based on this study we propose three mechanistic models for the Cu(II)-induced aggregation of A␤ 1-40 depending on the Cu(II):A␤ ratio, and identify key reaction steps that may be feasible targets for preventing Cu(II)-associated aggregation or toxicity in Alzheimer disease.Extracellular cerebral plaques composed mainly of amyloid ␤-peptide (A␤) 1-40 and 1-42 fibrils are a histopathological hallmark of Alzheimer disease (AD) 3 (1, 2). These plaques contain elevated levels of metals, in particular zinc and copper (3). Also, it has been shown that these metal ions can promote the aggregation of A␤ in vitro (4, 5). This implies a key role of the metal ions in the A␤-mediated pathology of AD (6), although the subject is still under much debate (7,8), and a role of amyloid-independent pathways in AD neurodegeneration have recently been reviewed (9).Specifically regarding the role of metal ions in the amyloidmediated pathology of AD, it is believed that Zn(II) acts as a neuroprotector (10, 11), whereas Cu(II) is considered to mediate neurotoxicity (12)(13)(14). The latter effect is thought to occur through early stage soluble A␤ and A␤-Cu oligomeric intermediates (15-18) that may be involved in the formation of reactive oxygen species (6). It was discovered that Cu(II) may be released postsynaptically at glutamatergic synapses in hippocampus (19,20), the site for initial A␤ deposition in AD. This provides an explanation for how Cu(II) can interact with A␤. Seemingly in contrast to the support for the neurotoxic effects of Cu(II),...

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Section: Cu(ii):a␤ 1-40 Ratiomentioning

confidence: 99%

Cu(II) Mediates Kinetically Distinct, Non-amyloidogenic Aggregation of Amyloid-β Peptides

Pedersen

Østergaard

Rozlosnik

et al. 2011

Journal of Biological Chemistry

118

160

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“…The experimental conditions for Ab 1-42 fibrillization have been described in previous reports. 7 The increase in the intensity of the fluorescence signal of ThT associated with Ab 1-42 fibrillization is depicted in Figure 8(A). The time course for the formation of the fibrils was also observed through continuous monitoring of the changes in the ThT fluorescence intensity at 480 nm over the course of 24 h; this time period is sufficient to allow fibril formation under incubation and stirring conditions.…”

Section: Evaluation Of Ab 1-42 Aggregation By Thioflavin T Fluorescencementioning

confidence: 99%

“…Some reports have demonstrated that the presence of Cu 21 favors fibril formation, 10 while other recent studies suggested that Cu 21 might inhibit Ab 1242 fibril formation. 7 In addition, numerous compounds have been found to reduce Ab 1242 aggregation in vitro. 11,12 However, the usefulness of these compounds as inhibitors of Ab 1242 aggregation remains speculative due to their lack of specificity and/or unknown mechanism of action.…”

Section: Introductionmentioning

confidence: 99%

“…One of the metals that has attracted attention is copper (Cu 21 ), whose concentration is threefold greater in AD patients than in normal patients, with concentrations between 340 and 400 mM. 6,7 The interaction between Ab-fibrils and Cu 21 is important not only because of its role in amyloidosis but also because it has been associated with the generation of oxidative stress. 8 Therefore, several experimental and computational methods have focused on the analysis of the interaction between Ab 1242 and Cu 21 .…”

Section: Introductionmentioning

confidence: 99%

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In silico and in vitro studies to elucidate the role of Cu²⁺ and galanthamine as the limiting step in the amyloid beta (1–42) fibrillation process

et al. 2013

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The formation of fibrils and oligomers of amyloid beta (Aβ) with 42 amino acid residues (Aβ1–42) is the most important pathophysiological event associated with Alzheimer's disease (AD). The formation of Aβ fibrils and oligomers requires a conformational change from an α‐helix to a β‐sheet conformation, which is encouraged by the formation of a salt bridge between Asp 23 or Glu 22 and Lys 28. Recently, Cu2+ and various drugs used for AD treatment, such as galanthamine (Reminyl®), have been reported to inhibit the formation of Aβ fibrils. However, the mechanism of this inhibition remains unclear. Therefore, the aim of this work was to explore how Cu2+ and galanthamine prevent the formation of Aβ1–42 fibrils using molecular dynamics (MD) simulations (20 ns) and in vitro studies using fluorescence and circular dichroism (CD) spectroscopies. The MD simulations revealed that Aβ1–42 acquires a characteristic U‐shape before the α‐helix to β‐sheet conformational change. The formation of a salt bridge between Asp 23 and Lys 28 was also observed beginning at 5 ns. However, the MD simulations of Aβ1−42 in the presence of Cu2+ or galanthamine demonstrated that both ligands prevent the formation of the salt bridge by either binding to Glu 22 and Asp 23 (Cu2+) or to Lys 28 (galanthamine), which prevents Aβ1−42 from adopting the U‐characteristic conformation that allows the amino acids to transition to a β‐sheet conformation. The docking results revealed that the conformation obtained by the MD simulation of a monomer from the 1Z0Q structure can form similar interactions to those obtained from the 2BGE structure in the oligomers. The in vitro studies demonstrated that Aβ remains in an unfolded conformation when Cu2+ and galanthamine are used. Then, ligands that bind Asp 23 or Glu 22 and Lys 28 could therefore be used to prevent β turn formation and, consequently, the formation of Aβ fibrils.

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“…D-penicillamine, a copper chelating molecule, was shown to have an interest for ADtargeted therapy [187,188] since metal ions such as iron or copper are involved in the formation AD pathogenesis due to the binding of APP, their accumulation in the AD brain [177,189,190]. This compound, already used in therapy of other pathologies such as the Wilson's disease affecting the liver, rheumatoidis and lead poisoning was tested as a nanoformulation where it was covalently linked to NPs in vitro and was successfully shown to disaggregate Aβ peptide [191].…”

Section: Therapeutic Strategies Using Nanoparticles In Ndmentioning

confidence: 99%

The Ins and Outs of Nanoparticle Technology in Neurodegenerative Diseases and Cancer

Wilson¹,

Magnaudeix²,

Naves³

et al. 2015

CDM

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Distinct Effects of Zn2+, Cu2+, Fe3+, and Al3+ on Amyloid-β Stability, Oligomerization, and Aggregation

Cited by 180 publications

References 73 publications

Cu(II) Mediates Kinetically Distinct, Non-amyloidogenic Aggregation of Amyloid-β Peptides

Cu(II) Mediates Kinetically Distinct, Non-amyloidogenic Aggregation of Amyloid-β Peptides

In silico and in vitro studies to elucidate the role of Cu²⁺ and galanthamine as the limiting step in the amyloid beta (1–42) fibrillation process

The Ins and Outs of Nanoparticle Technology in Neurodegenerative Diseases and Cancer

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Distinct Effects of Zn2+, Cu2+, Fe3+, and Al3+ on Amyloid-β Stability, Oligomerization, and Aggregation

Cited by 180 publications

References 73 publications

Cu(II) Mediates Kinetically Distinct, Non-amyloidogenic Aggregation of Amyloid-β Peptides

Cu(II) Mediates Kinetically Distinct, Non-amyloidogenic Aggregation of Amyloid-β Peptides

In silico and in vitro studies to elucidate the role of Cu2+ and galanthamine as the limiting step in the amyloid beta (1–42) fibrillation process

The Ins and Outs of Nanoparticle Technology in Neurodegenerative Diseases and Cancer

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In silico and in vitro studies to elucidate the role of Cu²⁺ and galanthamine as the limiting step in the amyloid beta (1–42) fibrillation process