Abstract:Brain copper imbalance plays an important role in amyloid-β aggregation, tau hyperphosphorylation, and neurotoxicity observed in Alzheimer's disease (AD). Therefore, the administration of biocompatible metal-binding agents may offer a potential therapeutic solution to target mislocalized copper ions and restore metallostasis. Histidine-containing peptides and proteins are excellent metal binders and are found in many natural systems. The design of short peptides showing optimal binding properties represents a … Show more
“…25,95 Therefore, the design of peptide-or peptidomimeticbased metal chelators/sequestrators has been an active area of research, although most of the reported chelators lack multifunctional features. 96,97 We developed the multifunctional peptidomimetic P6 by conjugating the copper-chelating natural tripeptide Gly-His-Lys (GHK) found in humans and the peptoid-based Ab aggregation modulator P5 (Fig. 7a and b).…”
Section: Targeting Ab and Tau Aggregationmentioning
The diverse pathological mechanisms and their implications for the development of effective diagnostic and therapeutic interventions in Alzheimer's disease are presented with current progress, challenges and future prospects.
“…25,95 Therefore, the design of peptide-or peptidomimeticbased metal chelators/sequestrators has been an active area of research, although most of the reported chelators lack multifunctional features. 96,97 We developed the multifunctional peptidomimetic P6 by conjugating the copper-chelating natural tripeptide Gly-His-Lys (GHK) found in humans and the peptoid-based Ab aggregation modulator P5 (Fig. 7a and b).…”
Section: Targeting Ab and Tau Aggregationmentioning
The diverse pathological mechanisms and their implications for the development of effective diagnostic and therapeutic interventions in Alzheimer's disease are presented with current progress, challenges and future prospects.
“…Possible configurations were built considering the information obtained from NMR experiments, [48] which indicated that the probable coordinating sites are the N term ,H is1, His3, and N À from the deprotonated amide of the backboneo rt he Of rom the carbonyl group of the backbone. Possible configurations were built considering the information obtained from NMR experiments, [48] which indicated that the probable coordinating sites are the N term ,H is1, His3, and N À from the deprotonated amide of the backboneo rt he Of rom the carbonyl group of the backbone.…”
Section: Electrochemical Properties Of Cu II -Tripeptidesmentioning
confidence: 99%
“…To determine which coordination mode provides the electrochemicalp roperties observed for these complexes,a nd to assessh ow much different coordination environments would influence the electrochemical behaviour,D FT (B3LYP-D3) calculationsw erec arried out for differentc onfigurations. Possible configurations were built considering the information obtained from NMR experiments, [48] which indicated that the probable coordinating sites are the N term ,H is1, His3, and N À from the deprotonated amide of the backboneo rt he Of rom the carbonyl group of the backbone. Since minor differences are expected among the two complexes, the exploration of different binding modes was first investigated for Cu II -HAH.F ourm ajor configurations werec onsidered from ac omputationalp oint of view: 1) configuration 1,i nvolving the N term ,H is1, His3, the carboxylate group, and the carbonyl Oo fA la2;2 )configuration 2,i nvolvingt he N term ,d eprotonated amide, the carbonyl Oo fA la2, and His3; 3) configuration 3,c orresponding to the ATCUN motif (see Scheme 1) and involving the N term ,H is3, andt he two deprotonated Na mides;a nd finally,4 )configuration 4,w ith His1, His3, the deprotonated N À amide, and the carbonyl Oo f Ala2 as binding sites.…”
Section: Electrochemical Properties Of Cu II -Tripeptidesmentioning
The binding and electrochemical properties of the complexes Cu -HAH, Cu -HWH, Cu -Ac-HWH, Cu -HHW, and Cu -WHH have been studied by using NMR and UV/Vis spectroscopies, CV, and density functional calculations. The results obtained highlight the importance of the peptidic sequence on the coordination properties and, consequently, on the redox properties of their Cu complexes. For Cu -HAH and Cu -HWH, no cathodic processes are observed up to -1.2 V; that is, the complexes exhibit very high stability towards copper reduction. This behaviour is associated with the formation of very stable square-planar (5,5,6)-membered chelate rings (ATCUN motif), which enclose two deprotonated amides. In contrast, for non-ATCUN Cu -Ac-HWH, Cu -HHW complexes, simulations seem to indicate that only one deprotonated amide is enclosed in the coordination sphere. In these cases, the main electrochemical feature is a reductive irreversible one electron-transfer process from Cu to Cu , accompanied with structural changes of the metal coordination sphere and reprotonation of the amide. Finally, for Cu -WHH, two major species have been detected: one at low pH (<5), with no deprotonated amides, and another one at high pH (>10) with an ATCUN motif, both species coexisting at intermediate pH. The present study shows that the use of CV, using glassy carbon as a working electrode, is an ideal and rapid tool for the determination of the redox properties of Cu metallopeptides.
“…However, in a longer 52-week trial, PBT2 did not reduce plaque burden or improve cognitive function to a statistically significant extent. Recently, Caballero and co-workers have designed peptide fragments containing one to two histidine residues which showed higher affinity for Cu 2+ ions than the Aβ40 peptide, and also showed reduced amyloid toxicity and reduced copper-generated ROS (Caballero et al 2016 ) (Fig. 3 i).…”
Section: Part 4: Metal Ionsmentioning
confidence: 99%
“… Fig. 3 Proposed molecules targeting Aβ aggregation: a heparin-based N-acetyl-glucosamine monosaccharide (Kisilevsky et al 2003 ); b Enoxaparin, a low-molecular-weight heparin (Bergamaschini et al 2004 ); c RNA aptamer β55 (Ylera et al 2002 ), with bases colored as shown; d RNA aptamer E2 (Rahimi et al 2009 ); e the statin Atorvastatin (Lipitor); f doxcosahexaenoic acid (DHA); g clioquinol; h PBT2; i tripeptide H-W-H (Caballero et al 2016 ) …”
Section: Introduction: What’s In a Plaque?mentioning
Aggregation of the amyloid-β (Aβ) peptide is strongly correlated with Alzheimer’s disease (AD). Recent research has improved our understanding of the kinetics of amyloid fibril assembly and revealed new details regarding different stages in plaque formation. Presently, interest is turning toward studying this process in a holistic context, focusing on cellular components which interact with the Aβ peptide at various junctures during aggregation, from monomer to cross-β amyloid fibrils. However, even in isolation, a multitude of factors including protein purity, pH, salt content, and agitation affect Aβ fibril formation and deposition, often producing complicated and conflicting results. The failure of numerous inhibitors in clinical trials for AD suggests that a detailed examination of the complex interactions that occur during plaque formation, including binding of carbohydrates, lipids, nucleic acids, and metal ions, is important for understanding the diversity of manifestations of the disease. Unraveling how a variety of key macromolecular modulators interact with the Aβ peptide and change its aggregation properties may provide opportunities for developing therapies. Since no protein acts in isolation, the interplay of these diverse molecules may differentiate disease onset, progression, and severity, and thus are worth careful consideration.
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