Natural Compounds against Alzheimer’s Disease: Molecular Recognition of Aβ1–42 Peptide by <i>Salvia sclareoides</i> Extract and its Major Component, Rosmarinic Acid, as Investigated by NMR

Airoldi, Cristina; Sironi, Erika; Dias, Catarina; Marcelo, Filipa; Martins, Alice; Rauter, Amélia P.; Nicotra, Francesco; Jiménez‐Barbero, Jesús

doi:10.1002/asia.201201063

Cited by 83 publications

(61 citation statements)

References 66 publications

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“…42 The normalized signal strengths (STD/STD reference) corresponding to each ligand atom are proportional to its proximity to the amyloid fibril, allowing an atomic-level map of the binding interactions from the ligand to the Aβ fibril to be made. 12 p ,41 The results from the STD NMR experiments indicate that both 1 and 4 interact fairly strongly (mM to μM dissociation constant) with the fibril to elicit a relatively strong STD signal (approximately 4.5% (for 1 ) and 5.9% (for 4 ) of the reference signal at a 3 sec saturation power of 50 dB, similar in magnitude to previous results with other catechols 41 ). The STD results also suggest that 1 and 4 bind similarly to the Aβ fibril (Fig.…”

Section: Resultssupporting

confidence: 85%

“…To probe these possible interactions, we employed saturation transfer difference (STD) NMR experiments to map the regions of the ligand which bind preformed fibrils of Aβ 40 (Fig. 8) 12 p ,41 and to visualize the potential contacts of 4 with Aβ fibrils, flexible ligand docking studies were employed with the solid state NMR structure of metal-free Aβ 40 (PDB 2LMN and 2LMO) (Figs. 8c, S9, and S10).…”

Section: Resultsmentioning

confidence: 99%

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Interaction and reactivity of synthetic aminoisoflavones with metal-free and metal-associated amyloid-β

et al. 2014

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Metal ion homeostasis in conjunction with amyloid-β (Aβ) aggregation in the brain has been implicated in Alzheimer’s disease (AD) pathogenesis. To uncover the interplay between metal ions and Aβ peptides, synthetic, multifunctional small molecules have been employed to modulate Aβ aggregation in vitro. Naturally occurring flavonoids have emerged as a valuable class of compounds for this purpose due to their ability to modulate both metal-free and metal-induced Aβ aggregation. Although, flavonoids have shown anti-amyloidogenic effects, the structural moieties of flavonoids responsible for such reactivity have not been fully identified. In order to understand the structure-interaction-reactivity relationship within the flavonoid family for metal-free and metal-associated Aβ, we designed, synthesized, and characterized a set of isoflavone derivatives, aminoisoflavones (1-4), that displayed reactivity (i.e., modulation of Aβ aggregation) in vitro. NMR studies revealed a potential binding site for aminoisoflavones between the N-terminal loop and central helix on prefibrillar Aβ different from the non-specific binding observed for other flavonoids. The absence or presence of the catechol group differentiated the binding affinities and enthalpy/entropy balance between aminoisoflavones and Aβ. Furthermore, having a catechol group influenced the binding mode with fibrillar Aβ. Inclusion of additional substituents moderately tuned the impact of aminoisoflavones on Aβ aggregation. Overall, through these studies, we obtained valuable insights on the requirements for parity among metal chelation, intermolecular interactions, and substituent variation for Aβ interaction.

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Section: Resultssupporting

confidence: 85%

Section: Resultsmentioning

confidence: 99%

Interaction and reactivity of synthetic aminoisoflavones with metal-free and metal-associated amyloid-β

et al. 2014

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“…STD experiments were acquired with a train of 60 dB Gaussian-shaped pulses of 50 ms duration at centered at either −2.0 ppm (on resonance 63–65 ) or 100 ppm (off resonance) with a total saturation time of 3 s on a Bruker 500 MHz (metal-free samples) or 900 MHz spectrometer (Zn( ii ) samples). 66 A total of 2048 transients with a 2 s recycle delay were collected for all spectra. Chemical shifts are referenced to water due to the potential interaction of Aβ40 with the chemical shift standard sodium 4,4-dimethyl-4-silapentane-1-sulfonate (DSS).…”

Section: Methodsmentioning

confidence: 99%

Rational Design of a Structural Framework with Potential Use to Develop Chemical Reagents That Target and Modulate Multiple Facets of Alzheimer’s Disease

et al. 2013

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Alzheimer’s disease (AD) is characterized by multiple, intertwined pathological features, including amyloid-β (Aβ) aggregation, metal ion dyshomeostasis, and oxidative stress. We report a novel compound (ML) prototype of a rationally designed molecule obtained by integrating structural elements for Aβ aggregation control, metal chelation, reactive oxygen species (ROS) regulation, and antioxidant activity within a single molecule. Chemical, biochemical, ion mobility mass spectrometric, and NMR studies indicate that the compound ML targets metal-free and metal-bound Aβ (metal–Aβ) species, suppresses Aβ aggregation in vitro, and diminishes toxicity induced by Aβ and metal-treated Aβ in living cells. Comparison of ML to its structural moieties (i.e., 4-(dimethylamino)phenol (DAP) and (8-aminoquinolin-2-yl)methanol (1)) for reactivity with Aβ and metal–Aβ suggests the synergy of incorporating structural components for both metal chelation and Aβ interaction. Moreover, ML is water-soluble and potentially brain permeable, as well as regulates the formation and presence of free radicals. Overall, we demonstrate that a rational structure-based design strategy can generate a small molecule that can target and modulate multiple factors, providing a new tool to uncover and address AD complexity.

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“…18,19 Among these, small organic molecules have received special interest because of their high permeability through the blood-brain barrier and potentially low cytotoxicity. 20 Several natural compounds have been found to prevent hIAPP brillization or to transform the mature brils into unstructured, off-pathway aggregates. 8,21,22 For example, Chen et al 23 have found that the brillation and aggregation of hIAPP is affected by trehalose in a dose-dependent manner.…”

Section: Introductionmentioning

confidence: 99%

Brazilin inhibits fibrillogenesis of human islet amyloid polypeptide, disassembles mature fibrils, and alleviates cytotoxicity

Guo

Sun

et al. 2017

RSC Adv.

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Fibrillogenesis of human islet amyloid polypeptide (hIAPP) is a pathological hallmark of type II diabetes mellitus (T2DM), and the inhibition of hIAPP fibrillogenesis is an important strategy for the prevention and treatment of T2DM. In this study, the inhibitory effects of brazilin on the fibrillization and cytotoxicity of hIAPP were examined using the thioflavin T fluorescence (ThT) assay, transmission electron microscopy (TEM), circular dichroism (CD) spectroscopy, cytotoxicity assays, and molecular dynamics simulations.Both the ThT and TEM results have shown that brazilin inhibits hIAPP fibrillogenesis in a dose-dependent manner. CD studies revealed that brazilin delays the conformational transition of hIAPP from its initial ahelical to the b-sheet form. As a result, brazilin greatly alleviates hIAPP-induced cytotoxicity. Moreover, we also found that brazilin disassembles preexisting hIAPP fibrils, and alleviates the cytotoxicity of hIAPP aggregates. The results of free energy decomposition studies calculated using molecular mechanicsPoisson-Boltzmann surface area analysis revealed that hydrophobic interactions contribute more than 75% of the free energy of binding in the brazilin-hIAPP complex, while electrostatic interactions (i.e., hydrogen bonds) play a secondary role (<25%). Two binding sites of brazilin on the hIAPP pentamer were identified, encompassing the N-terminal region and the turn region. There are 11 important residues of hIAPP that strongly interact with brazilin -Asn3, Thr4, Thr9, Arg11, Asn14, Phe15, His18, Ser19, Ser20, Asn21 and Phe23. The findings presented here will contribute to a comprehensive understanding of the inhibitory effect of brazilin on the fibrillogenesis of hIAPP, which is critical for the search for more effective agents that can inhibit hIAPP fibrillogenesis.

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Natural Compounds against Alzheimer’s Disease: Molecular Recognition of Aβ1–42 Peptide by Salvia sclareoides Extract and its Major Component, Rosmarinic Acid, as Investigated by NMR

Cited by 83 publications

References 66 publications

Interaction and reactivity of synthetic aminoisoflavones with metal-free and metal-associated amyloid-β

Interaction and reactivity of synthetic aminoisoflavones with metal-free and metal-associated amyloid-β

Rational Design of a Structural Framework with Potential Use to Develop Chemical Reagents That Target and Modulate Multiple Facets of Alzheimer’s Disease

Brazilin inhibits fibrillogenesis of human islet amyloid polypeptide, disassembles mature fibrils, and alleviates cytotoxicity

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