Navigating α‐Synuclein Aggregation Inhibition: Methods, Mechanisms, and Molecular Targets

Galkin, Maksym; Priss, Anastasiia; Kyriukha, Yevhenii; Shvadchak, Volodymyr

doi:10.1002/tcr.202300282

Cited by 5 publications

(4 citation statements)

References 224 publications

(342 reference statements)

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“…The current status of a Parkinson's disease treatment by using inhibitors of α-synuclein fibrillization process is reviewed by Galkin, Shvadchak, and co-workers. [20] Special attention is paid to the specificity of inhibitors and critical analysis of their action mechanisms. The authors also compare strategies of targeting monomeric, oligomeric, and fibrillar α-synuclein species, thoroughly discussing the strong and weak sides of different approaches to testing the inhibitors.…”

Section: Valentynmentioning

confidence: 99%

Chemistry in Ukraine

Grygorenko,

Lampeka,

Chebanov

et al. 2024

The Chemical Record

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In this special issue, we highlight recent advances in chemical research by scientists in Ukraine, as well as by their compatriots and collaborators outside the country. Besides spotlighting their contributions, we see our task in fostering global partnerships and multi‐, inter‐, and trans‐disciplinary collaborations, including much‐needed co‐funded projects and initiatives. The three decades of the renewed Ukraine independence have seen rather limited integration of Ukrainian (chemical) science into global research communities. [1] At the same time, the recent surge of collaborative science initiatives between European Union (EU) and Ukraine echoes the unfolding steps towards Ukraine's full research participation to the Horizon Europe Program. This recently implemented step opens enormous possibilities for Ukrainian researchers to apply for diverse EU research grants. Moreover, a number of journal special issues and collections were launched to highlight Ukrainian chemistry (i. e., by Chemistry of Heterocyclic Compounds [2] and ChemistrySelect [3]). Other scientific initiatives include ‘European Chemistry School for Ukrainians’ [4] and ‘Kharkiv Chemical Seminar’ [5] as voluntary projects aimed at engaging Ukrainian scientists into European and international chemical research.

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Section: Valentynmentioning

confidence: 99%

Chemistry in Ukraine

Grygorenko,

Lampeka,

Chebanov

et al. 2024

The Chemical Record

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“…A promising avenue involves the identification of small molecules with anti-αSyn aggregation or stress-alleviating properties. Currently, a number of small-molecule inhibitors of αSyn aggregation from synthetic sources have been discovered, mostly through high-throughput screening strategies (e.g., [24][25][26]). However, plants offer another screening palette for the identification of aggregation inhibitors, expanding the potential pool of compounds that may hold therapeutic promise.…”

Section: Introductionmentioning

confidence: 99%

A Plant Model of α-Synucleinopathy: Expression of α-Synuclein A53T Variant in Hairy Root Cultures Leads to Proteostatic Stress and Dysregulation of Iron Metabolism

Kurepa,

Bruce,

Gerhardt

et al. 2024

Applied Biosciences

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Synucleinopathies, typified by Parkinson’s disease (PD), entail the accumulation of α-synuclein (αSyn) aggregates in nerve cells. Various αSyn mutants, including the αSyn A53T variant linked to early-onset PD, increase the propensity for αSyn aggregate formation. In addition to disrupting protein homeostasis and inducing proteostatic stress, the aggregation of αSyn in PD is associated with an imbalance in iron metabolism, which increases the generation of reactive oxygen species and causes oxidative stress. This study explored the impact of αSyn A53T expression in transgenic hairy roots of four medicinal plants (Lobelia cardinalis, Artemisia annua, Salvia miltiorrhiza, and Polygonum multiflorum). In all tested plants, αSyn A53T expression triggered proteotoxic stress and perturbed iron homeostasis, mirroring the molecular profile observed in human and animal nerve cells. In addition to the common eukaryotic defense mechanisms against proteostatic and oxidative stresses, a plant stress response generally includes the biosynthesis of a diverse set of protective secondary metabolites. Therefore, the hairy root cultures expressing αSyn A53T offer a platform for identifying secondary metabolites that can ameliorate the effects of αSyn, thereby aiding in the development of possible PD treatments and/or treatments of synucleinopathies.

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“…Heat shock proteins (HSPs) and proteins from endoplasmic reticulum play an important role in maintaining cellular protein homeostasis and can protect neurons from damage by degradation of aggregates through different mechanisms [10,11]. Therefore, in the search for new therapeutic strategies, α-synuclein aggregation and misfolding are considered a priority target for drug development [12][13][14].…”

Section: Introductionmentioning

confidence: 99%

The 75–99 C-Terminal Peptide of URG7 Protein Promotes α-Synuclein Disaggregation

Dandurand,

Monné,

Samouillan

et al. 2024

IJMS

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Up Regulation Gene seven (URG7) is the pseudogene 2 of the transporter ABCC6. The translated URG7 protein is localized with its single transmembrane α-helix in the endoplasmic reticulum (ER) membrane, orienting the N- and C-terminal regions in the lumen and cytoplasm, respectively, and it plays a crucial role in the folding of ER proteins. Previously, the C-terminal region of URG7 (PU, residues 75–99) has been shown to modify the aggregation state of α-synuclein in the lysate of HepG2 cells. PU analogs were synthesized, and their anti-aggregation potential was tested in vitro on α-synuclein obtained using recombinant DNA technology. Circular dichroism (CD), differential scanning calorimetry (DSC), Fourier-transform infrared (FTIR) spectroscopy, and microscopic techniques were used to assess the sample’s behavior. The results show that the peptides studied by themselves are prone to clathrate-like structure formation of variable stability. Aggregation of α-synuclein is accompanied by desolvation of its peptide chain and an increase in intermolecular β-sheets. The PU analogs all interact with α-synuclein aggregates and those possessing the most stable clathrate-like structures have the highest disaggregating effect. These findings suggest that the C-terminal region of URG7 may have a role in interacting and modulating α-synuclein structures and could be used to generate interesting therapeutic candidates as disaggregators of α-synuclein.

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Navigating α‐Synuclein Aggregation Inhibition: Methods, Mechanisms, and Molecular Targets

Cited by 5 publications

References 224 publications

Chemistry in Ukraine

Chemistry in Ukraine

A Plant Model of α-Synucleinopathy: Expression of α-Synuclein A53T Variant in Hairy Root Cultures Leads to Proteostatic Stress and Dysregulation of Iron Metabolism

The 75–99 C-Terminal Peptide of URG7 Protein Promotes α-Synuclein Disaggregation

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