Real‐Time BODIPY‐Binding Assay To Screen Inhibitors of the Early Oligomerization Process of Aβ1–42 Peptide

Tonali, Nicolò; Dodero, Verónica Isabel; Kaffy, Julia; Hericks, Loreen; Ongeri, Sandrine; Sewald, Norbert

doi:10.1002/cbic.201900652

Cited by 19 publications

(25 citation statements)

References 41 publications

(55 reference statements)

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“…These probes interact with high sensitivity with Aβ-peptide fibrils, showing an increment in their fluorescence emission, and some of them, such as CRANAD probes, suffer a blue-shift of the maximum of the emission upon binding. Recently, a Triazole-BODIPY-based probe was shown to detect, in a time-dependent manner, the first stages of Aβ-peptide oligomerization before fibril formation [ 104 ]. Additionally, the same BODIPY derivative identified the presence of oligomers of the toxic p31–43 peptide related to celiac disease [ 49 ].…”

Section: Fluorescence Spectroscopy Is a Versatile Tool For Evaluatmentioning

confidence: 99%

“…CD is widely used to evaluate the formation of amyloid fibrils at different experimental conditions such as time, changes in pH, and presence of different molecules, among others. The Aβ-peptide [ 104 ], the Ac-Phe-Phe-Cys-NH 2 (Ac-FFC-NH 2 ) amyloid peptide model [ 61 ], and proteins such as alpha-synuclein [ 152 ] and β2-microglobulin [ 153 ] have been shown to change their conformation from random coil to β-sheet structure over time during the aggregation process, which is compatible with the formation of fibrils. Other systems, such as the rationally designed DN1 peptide, have been shown to self-aggregate into fibrils in a concentration-dependent manner [ 154 ].…”

Section: Circular Dichroism Makes It Possible To Follow Secondary mentioning

confidence: 99%

“…In 0 (black), 0.5 (red), 1 (violet) 3 (blue) and 7 h (green). This image was extracted and re-created from Tonali et al [ 104 ]. ( B ) Spectra showing the structural transformation of the 33-mer gliadin peptide at 613 µM depending the temperature, at −5 °C (red) corresponds to PPII structure and at 37 °C (black) to the β-sheet signature.…”

Section: Figurementioning

confidence: 99%

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Evaluation of Peptide/Protein Self-Assembly and Aggregation by Spectroscopic Methods

2020

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The self-assembly of proteins is an essential process for a variety of cellular functions including cell respiration, mobility and division. On the other hand, protein or peptide misfolding and aggregation is related to the development of Parkinson’s disease and Alzheimer’s disease, among other aggregopathies. As a consequence, significant research efforts are directed towards the understanding of this process. In this review, we are focused on the use of UV-Visible Absorption Spectroscopy, Fluorescence Spectroscopy and Circular Dichroism to evaluate the self-organization of proteins and peptides in solution. These spectroscopic techniques are commonly available in most chemistry and biochemistry research laboratories, and together they are a powerful approach for initial as well as routine evaluation of protein and peptide self-assembly and aggregation under different environmental stimulus. Furthermore, these spectroscopic techniques are even suitable for studying complex systems like those in the food industry or pharmaceutical formulations, providing an overall idea of the folding, self-assembly, and aggregation processes, which is challenging to obtain with high-resolution methods. Here, we compiled and discussed selected examples, together with our results and those that helped us better to understand the process of protein and peptide aggregation. We put particular emphasis on the basic description of the methods as well as on the experimental considerations needed to obtain meaningful information, to help those who are just getting into this exciting area of research. Moreover, this review is particularly useful to those out of the field who would like to improve reproducibility in their cellular and biomedical experiments, especially while working with peptide and protein systems as an external stimulus. Our final aim is to show the power of these low-resolution techniques to improve our understanding of the self-assembly of peptides and proteins and translate this fundamental knowledge in biomedical research or food applications.

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Section: Fluorescence Spectroscopy Is a Versatile Tool For Evaluatmentioning

confidence: 99%

Section: Circular Dichroism Makes It Possible To Follow Secondary mentioning

confidence: 99%

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Evaluation of Peptide/Protein Self-Assembly and Aggregation by Spectroscopic Methods

2020

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“…Aggregates of toxic Aβ in the form of soluble Aβ oligomers, intraneuronal Aβ, and amyloid plaques injure the synapses and ultimately cause neurodegeneration and dementia [6,7]. One of the strategies adopted to stop or reverse the progression of the disease is to modulate or inhibit the aggregation process of Aβ, by various mechanisms: stabilization of its native state, destabilization of its incorrectly folded state [8], bypass of the on-pathway oligomer formation, inhibition of the fibril elongation and disaggregation of the already formed amyloid aggregates [9][10][11][12].…”

Section: Introductionmentioning

confidence: 99%

“…Instead, the second class is characterized by peptides which are identified from libraries, that may or may not show sequence similarly to wild type, and these are termed as randomly generated peptides. Other approaches have been exploited in the field of peptidomimetics, such as synthetic peptide derivates-β sheet breakers and β peptide hairpins [9][10][11][12].…”

Section: Introductionmentioning

confidence: 99%

The Positive Side of the Alzheimer’s Disease Amyloid Cross-Interactions: The Case of the Aβ 1-42 Peptide with Tau, TTR, CysC, and ApoA1

et al. 2020

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Alzheimer’s disease (AD) represents a progressive amyloidogenic disorder whose advancement is widely recognized to be connected to amyloid-β peptides and Tau aggregation. However, several other processes likely contribute to the development of AD and some of them might be related to protein-protein interactions. Amyloid aggregates usually contain not only single type of amyloid protein, but also other type of proteins and this phenomenon can be rationally explained by the process of protein cross-seeding and co-assembly. Amyloid cross-interaction is ubiquitous in amyloid fibril formation and so a better knowledge of the amyloid interactome could help to further understand the mechanisms of amyloid related diseases. In this review, we discuss about the cross-interactions of amyloid-β peptides, and in particular Aβ1-42, with other amyloids, which have been presented either as integrated part of Aβ neurotoxicity process (such as Tau) or conversely with a preventive role in AD pathogenesis by directly binding to Aβ (such as transthyretin, cystatin C and apolipoprotein A1). Particularly, we will focus on all the possible therapeutic strategies aiming to rescue the Aβ toxicity by taking inspiration from these protein-protein interactions.

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Peptidotriazolamers Inhibit Aβ(1–42) Oligomerization and Cross a Blood‐Brain‐Barrier Model

et al. 2021

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In peptidotriazolamers every second peptide bond is replaced by a 1H-1,2,3-triazole. Such foldamers are expected to bridge the gap in molecular weight between small-molecule drugs and protein-based drugs. Amyloid β (Aβ) aggregates play an important role in Alzheimer's disease. We studied the impact of amide bond replacements by 1,4-disubstituted 1H-1,2,3-triazoles on the inhibitory activity of the aggregation "hot spots" K 16 LVFF 20 and G 39 VVIA 42 in Aβ(1-42). We found that peptido-triazolamers act as modulators of the Aβ(1-42) oligomerization. Some peptidotriazolamers are able to interfere with the formation of toxic early Aβ oligomers, depending on the position of the triazoles, which is also supported by computational studies. Preliminary in vitro results demonstrate that a highly active peptidotriazolamer is also able to cross the bloodbrain-barrier.

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Real‐Time BODIPY‐Binding Assay To Screen Inhibitors of the Early Oligomerization Process of Aβ1–42 Peptide

Cited by 19 publications

References 41 publications

Evaluation of Peptide/Protein Self-Assembly and Aggregation by Spectroscopic Methods

Evaluation of Peptide/Protein Self-Assembly and Aggregation by Spectroscopic Methods

The Positive Side of the Alzheimer’s Disease Amyloid Cross-Interactions: The Case of the Aβ 1-42 Peptide with Tau, TTR, CysC, and ApoA1

Peptidotriazolamers Inhibit Aβ(1–42) Oligomerization and Cross a Blood‐Brain‐Barrier Model

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