Journal ArticleDOI
Impact of the Acidic C-Terminal Region Comprising Amino Acids 109−140 on α-Synuclein Aggregation in Vitro†
TLDR
The effects of the C-terminus on aggregation cannot be rationalized merely by a contribution to the protein net charge, but rather suggest a specific role of aa109-140 in the regulation of aggregation, presumably involving formation of intramolecular contacts.Abstract:
The aggregation of alpha-synuclein, involved in the pathogenesis of several neurodegenerative disorders such as Parkinson's disease, is enhanced in vitro by biogenic polyamines binding to the highly charged C-terminal region aa109-140. In this study, we investigated the influence of this region on the aggregation kinetics, monitored by thioflavin T binding and static light scattering, and morphology, assessed by electron microscopy, fluorescence microscopy, and turbidity, by comparing the effect of various solution conditions on the wild-type protein, the disease related mutants A53T and A30P, and two truncated variants, syn(1-108) and syn(1-124), lacking the complete or the C-terminal half of the polyamine binding site. In the presence of the intact C-terminus, aggregation was strongly retarded in physiological buffer. This inhibition of aggregation was overridden by (i) addition of spermine or MgCl(2) or lowering of pH, leading to strong charge shielding in the C-terminus or (ii) by truncation of aa125-140 or aa109-140. Addition of MgCl(2) or spermine or acidification were not effective in promoting aggregation of syn(1-108). The impact of the disease-related mutations on the aggregation kinetics was dependent on the solution conditions, with the aggregation propensity order A53T approximately wt > A30P at low ionic strength, but A53T > wt approximately A30P at high ionic strength, with exceedingly potent promotion of aggregation by the A53T mutation in the presence of spermine. In contrast to full-length alpha-synuclein aggregates, those formed from syn(1-108) did not exhibit a pronounced polymorphism. The effects of the C-terminus on aggregation cannot be rationalized merely by a contribution to the protein net charge, but rather suggest a specific role of aa109-140 in the regulation of aggregation, presumably involving formation of intramolecular contacts.read more
Citations
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Journal ArticleDOI
How Full-Length FVIII Benefits from Its Heterogeneity – Insights into the Role of the B-Domain
Julia Anzengruber,Martin Feichtinger,Philipp Bärnthaler,Norbert Haider,Josenato Ilas,Nina Pruckner,Karima Benamara,Friedrich Scheiflinger,Birgit M. Reipert,Mantas Malisauskas +9 more
TL;DR: These results demonstrate that pdFVIII and FL-rFV III have similar levels of molecular heterogeneity, and suggest that heterogeneity and the B-domain are involved in stabilising FVIII by modulating its aggregation pathway.
Dissertation
Multiple system atrophy : a translational approach Characterization of the insulin/IGF-1 signaling pathway
TL;DR: In this article, translational approaches in synucleinopathies and more specifically in multiple system atrophy (MSA) were focused on translational approach in the brain and showed that α-synuclein (α-syn) truncation pharmacologically in MSA transgenic mice led to reduced αsyn aggregation and the protection of dopaminergic neurons.
Dissertation
Alpha-synuclein spreading pathology in Parkinson's disease: the influence of iron and the Rho-kinase inhibitor fasudil
TL;DR: The present work investigates the influence of trace elements, particularly iron, and ROCK inhibition on α-syn spreading and contributes to a better understanding of PD pathophysiology and to the identification of auspicious targets for new therapeutic strategies.
Journal ArticleDOI
C-terminal truncation of α-synuclein alters DNA structure from extension to compaction.
TL;DR: In this article, the role of negatively-charged C-terminus in the interaction between α-synuclein and DNA using single-molecule techniques was investigated using nanofluidic channels, and it was shown that truncation of the Cterminus of aS induces differential effects on DNA depending on the extent of the truncation.
Book ChapterDOI
Interaction of alpha-synuclein with lipids.
TL;DR: A comprehensive understanding of the factors that modulate these interactions will help delineate the physiological and pathological states of α-synuclein (α-syn) protein this paper , which is a natively unfolded protein that is abundantly expressed in the central nervous system.
References
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Journal ArticleDOI
Accelerated in vitro fibril formation by a mutant alpha-synuclein linked to early-onset Parkinson disease.
TL;DR: It is demonstrated that at higher concentrations, Lewy body-like fibrils and discrete spherical assemblies are formed; most rapidly by A53T, suggesting mutation-induced acceleration of α-synuclein fibril formation may contribute to the early onset of familial PD.
Journal ArticleDOI
Fibrils Formed in Vitro from α-Synuclein and Two Mutant Forms Linked to Parkinson's Disease are Typical Amyloid†
TL;DR: Fibrils generated in vitro from alpha-synuclein, wild-type and both mutant forms, are shown to possess very similar features that are characteristic of amyloid fibrils, including a wound and predominantly unbranched morphology, distinctive dye-binding properties, and antiparallel beta-sheet structure.
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