Small Molecules Attenuate the Interplay between Conformational Fluctuations, Early Oligomerization and Amyloidosis of Alpha Synuclein

Krishnananda Chattopadhyay,Sumanta Ghosh,Amrita Kundu

doi:10.1038/s41598-018-23718-3

Krishnananda Chattopadhyay, Sumanta Ghosh + Show 1 more

Open Access

https://doi.org/10.1038/s41598-018-23718-3

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Journal: Scientific Reports	Publication Date: Apr 3, 2018
Citations: 26	License type: open-access

Affiliation: Indian Institute of Chemical Biology

Abstract

Aggregation of alpha synuclein has strong implications in Parkinson’s disease. The heterogeneity of folding/aggregation landscape and transient nature of the early intermediates result in difficulty in developing a successful therapeutic intervention. Here we used fluorescence measurements at ensemble and single molecule resolution to study how the late and early events of alpha synuclein aggregation modulate each other. In-vitro aggregation data was complemented using measurements inside live neuroblastoma cells by employing a small molecule labeling technique. An inhibitor molecule (arginine), which delayed the late event of amyloidosis, was found to bind to the protein, shifting the early conformational fluctuations towards a compact state. In contrast, a facilitator of late aggregation (glutamate), was found to be excluded from the protein surface. The presence of glutamate was found to speed up the oligomer formation at the early stage. We found that the effects of the inhibitor and facilitator were additive and as a result they maintained a ratio at which they cancelled each other’s influence on different stages of alpha synuclein aggregation.

Highlights

The most widely studied component of α-syn aggregation kinetics is the late stage, at which the formation of amyloid fibrils takes place
The results obtained in the present study showed that the competition between conformational fluctuations and oligomerization could be a key factor in defining the folding-aggregation landscape of α-syn
Using isothermal calorimetry (ITC) and mass spectroscopy, we found out that the effect of arginine was probably due to the binding of multimeric arginine onto the protein molecules, while glutamate remained excluded

Summary

Introduction

The most widely studied component of α-syn aggregation kinetics is the late stage, at which the formation of amyloid fibrils (component 3) takes place. Results and Discussion In-vitro and live cell data suggest that arginine is an inhibitor and glutamate is a facilitator for the late stage of aggregation.

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Results

Conclusion