Multistep Inhibition of α-Synuclein Aggregation and Toxicity <i>in Vitro</i> and <i>in Vivo</i> by Trodusquemine

Perni, Michele; Flagmeier, Patrick; Limbocker, Ryan; Cascella, Roberta; Aprile, Francesco A.; Galvagnion, Céline; Heller, Gabriella T.; Meisl, Georg; Chen, Serene W.; Kumita, Janet R.; Challa, Pavan Kumar; Kirkegaard, Julius B.; Cohen, Samuel I.; Mannini, Benedetta; Barbut, Denise; Nollen, Ellen A. A.; Cecchi, Cristina; Cremades, Nunilo; Knowles, Tuomas P. J.; Chiti, Fabrizio; Zasloff, Michael; Vendruscolo, Michele

doi:10.1021/acschembio.8b00466

Cited by 95 publications

(168 citation statements)

References 67 publications

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“…Such compounds have the potential to serve in a therapeutic capacity by targeting specifically the microscopic steps of Aβ 42 that are responsible for oligomer production and proliferation [15][16][17][18][19] . Similar strategies have been employed to identify species that inhibit oligomer formation by αS, in particular by targeting the microscopic step of fibril amplification [20][21][22] .…”

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confidence: 99%

“…Despite the distinct mechanisms of the aggregation of αS and Aβ 42 and the differing effects of trodusquemine on the underlying processes, however, these effects resulted in a lower steady-state concentration of oligomers in both cases, in spite of the accelerated overall aggregation process in the case of Aβ 42 28 . Moreover, this molecule was found to suppress the toxic effects of both αS and Aβ 42 oligomers in cultured human neuroblastoma cells by markedly reducing the affinity of these aggregates for the cell membrane 20,28 . We also found that squalamine, an aminosterol comparable in structure to trodusquemine but with one less positive charge in its polyamine chain, similarly reduces the toxicity of αS oligomers to cells by their displacement from cell membranes 22 .…”

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confidence: 99%

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Trodusquemine displaces protein misfolded oligomers from cell membranes and abrogates their cytotoxicity through a generic mechanism

et al. 2020

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The onset and progression of numerous protein misfolding diseases are associated with the presence of oligomers formed during the aberrant aggregation of several different proteins, including amyloid-β (Aβ) in Alzheimer's disease and α-synuclein (αS) in Parkinson's disease. These small, soluble aggregates are currently major targets for drug discovery. In this study, we show that trodusquemine, a naturally-occurring aminosterol, markedly reduces the cytotoxicity of αS, Aβ and HypF-N oligomers to human neuroblastoma cells by displacing the oligomers from cell membranes in the absence of any substantial morphological and structural changes to the oligomers. These results indicate that the reduced toxicity results from a mechanism that is common to oligomers from different proteins, shed light on the origin of the toxicity of the most deleterious species associated with protein aggregation and suggest that aminosterols have the therapeutically-relevant potential to protect cells from the oligomer-induced cytotoxicity associated with numerous protein misfolding diseases.

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Trodusquemine displaces protein misfolded oligomers from cell membranes and abrogates their cytotoxicity through a generic mechanism

et al. 2020

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“…74 However, the concentration of Ca 2+ required to induce a-synuclein aggregation in free solution is far higher than that required in order to induce aggregation at a hydrophobic glass surface. 74 For a binding site of Ca 2+ , study shows that Ca 2+ binds to the C-terminal domain (126)(127)(128)(129)(130)(131)(132)(133)(134)(135)(136)(137)(138)(139)(140) however, currently there is no information which particular residue is involved in the binding process. 74 There is currently a lack of information about the effect of Pb on aggregation in vitro, although it has been demonstrated that Zn 2+ , Al 3+ and Pb 2+ enable methionineoxidized a-synuclein, 75 to form aggregates at the same rate as the non-oxidized a-synuclein.…”

Section: A-synucleinmentioning

confidence: 99%

“…Understanding how protein aggregation works has led some scientists to develop anti-aggregation drugs against TP and a-synuclein. [134][135][136] More systematic experiments designed to clarify this relationship are vital, as they may provide the groundwork to produce better therapeutics. Therefore, further research with more rigorous and detailed studies are necessary to denitively uncover the relationship between metal ions and their effects on the aggregation of proteins, with a particular emphasis on their concentrations and relative ratios.…”

Section: Conclusion and Future Outlookmentioning

confidence: 99%

Aggregation of biologically important peptides and proteins: inhibition or acceleration depending on protein and metal ion concentrations

et al. 2020

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“…Recently, a squalamine derivative, called trodusquemine, has been shown to affect the aggregation of α-syn as well [ 36 ]. In addition to displacing α-syn monomers similar to the mechanism fulfilled by squalamine, trodusquemine directly interacts with α-syn to inhibit the secondary nucleation of aggregation [ 36 ].…”

Section: The Main Classes Of Anti-amyloid Compoundsmentioning

confidence: 99%

Targeting Amyloid Aggregation: An Overview of Strategies and Mechanisms

Giorgetti

Greco

Tortora

et al. 2018

IJMS

111

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Amyloids result from the aggregation of a set of diverse proteins, due to either specific mutations or promoting intra- or extra-cellular conditions. Structurally, they are rich in intermolecular β-sheets and are the causative agents of several diseases, both neurodegenerative and systemic. It is believed that the most toxic species are small aggregates, referred to as oligomers, rather than the final fibrillar assemblies. Their mechanisms of toxicity are mostly mediated by aberrant interactions with the cell membranes, with resulting derangement of membrane-related functions. Much effort is being exerted in the search for natural antiamyloid agents, and/or in the development of synthetic molecules. Actually, it is well documented that the prevention of amyloid aggregation results in several cytoprotective effects. Here, we portray the state of the art in the field. Several natural compounds are effective antiamyloid agents, notably tetracyclines and polyphenols. They are generally non-specific, as documented by their partially overlapping mechanisms and the capability to interfere with the aggregation of several unrelated proteins. Among rationally designed molecules, we mention the prominent examples of β-breakers peptides, whole antibodies and fragments thereof, and the special case of drugs with contrasting transthyretin aggregation. In this framework, we stress the pivotal role of the computational approaches. When combined with biophysical methods, in several cases they have helped clarify in detail the protein/drug modes of interaction, which makes it plausible that more effective drugs will be developed in the future.

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Multistep Inhibition of α-Synuclein Aggregation and Toxicity in Vitro and in Vivo by Trodusquemine

Cited by 95 publications

References 67 publications

Trodusquemine displaces protein misfolded oligomers from cell membranes and abrogates their cytotoxicity through a generic mechanism

Trodusquemine displaces protein misfolded oligomers from cell membranes and abrogates their cytotoxicity through a generic mechanism

Aggregation of biologically important peptides and proteins: inhibition or acceleration depending on protein and metal ion concentrations

Targeting Amyloid Aggregation: An Overview of Strategies and Mechanisms

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