4.6 Article

Structural changes in α-synuclein affect its chaperone-like activity in vitro

Journal

PROTEIN SCIENCE
Volume 9, Issue 12, Pages 2489-2496

Publisher

CAMBRIDGE UNIV PRESS
DOI: 10.1110/ps.9.12.2489

Keywords

alpha-synuclein; molecular chaperone; Parkinson's disease; protein folding; structural change

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alpha -Synuclein, a major constituent of Lewy bodies (LBs) in Parkinson's disease (PD), has been implicated to play a critical role in synaptic events, such as neuronal plasticity during development, learning, and degeneration under pathological conditions, although the physiological function of alpha -synuclein has not yet been established. We here present biochemical evidence that recombinant alpha -synuclein has a chaperone-like function against thermal and chemical stress in vitro. In our experiments, alpha -synuclein protected glutathione S-transferase (GST) and aldolase from heat-induced precipitation, and alpha -lactalbumin and bovine serum albumin from dithiothreitol (DTT)-induced precipitation like other molecular chaperones. Moreover, preheating of alpha -synuclein, which is believed to reorganize the molecular surface of alpha -synuclein, increased the chaperone-like activity. Interestingly, in organic solvents, which promotes the formation of secondary structure, alpha -synuclein aggregated more easily than in its native condition, which eventually might abrogate the chaperone-like function of the protein. In addition, alpha -synuclein was also rapidly and significantly precipitated by heat in the presence of Zn2+ in vitro, whereas it was not affected by the presence of Ca2+ or Mg2+. Circular dichroism spectra confirmed that alpha -synuclein underwent conformational change in the presence of Zn2+. Taken together, our data suggest that alpha -synuclein could act as a molecular chaperone, and that the conformational change of the alpha -synuclein could explain the aggregation kinetics of alpha -synuclein, which may be related to the abolishment of the chaperonic-like activity.

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