University of Illinois Chicago
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Interaction between Alpha-Synuclein and Psychosine: Implications for Lewy Body Formation

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posted on 2014-10-28, 00:00 authored by Marta B. Santos
TITLE: INTERACTION BETWEEN ALPHA SYNUCLEIN AND PSYCHOSINE: IMPLICATIONS FOR LEWY BODY FORMATION. Alpha-synuclein is a protein implicated in an increasing number of diseases. Protein aggregates containing alpha-synuclein known as Lewy bodies, are typically found in Parkinson’s disease and other synucleionopathies. We have found that psychosine accelerates the fibrillization of alpha-synuclein in vitro in a dose-dependent manner. Psychosine is a cationic sphingolipid implicated in Krabbe disease, a lysosomal storage disorder, in which excess of psychosine (D-Galactosylsphingosine) causes severe CNS damages. Also, we found similarities between Krabbe disease and Parkinson’s that are consistent with synucleionopathy hallmarks. Using NMR and ITC measurements, we show that psychosine is a direct ligand of alpha-synuclein and thus of therapeutic interest. This work characterizes the binding sites, affinity and stoichiometry of this interaction. It also reveals individual residue contributions assigned at both N and C-terminals of alpha-synuclein. We find that psychosine may act as alpha-synuclein cross-linker and a C-terminal neutralizing agent. These observations suggest that binding of psychosine triggers aggregation and fibril expansion due to thermodynamically unfavorable and kinetically favorable interactions that remove the energy barriers to alpha-synuclein fibrillization-aggregation formation. Investigating how ligand binding accelerates alpha-synuclein fibrillization is crucial to understanding how alpha-synuclein goes from the soluble to the Lewy body amyloidogenic state. This work contributes to the growing field of protein deposition disorders.

History

Advisor

Bongarzone, Ernesto R.

Department

Anatomy and Cell Biology

Degree Grantor

University of Illinois at Chicago

Degree Level

  • Doctoral

Committee Member

Givogri, Maria I. Art, Jonathan J. Gaponenko, Vadim

Submitted date

2014-08

Language

  • en

Issue date

2014-10-28

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