Tissue transglutaminase modulates {alpha}-synuclein oligomerization

doi:10.1110/ps.036103.108

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Published online before print May 27, 2008, 10.1110/ps.036103.108
Protein Science (2008), 17:1395-1402. Published by Cold Spring Harbor Laboratory Press. Copyright © 2008 The Protein Society

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Tissue transglutaminase modulates ${alpha}$ -synuclein oligomerization

Ine M.J. Segers-Nolten¹, Micha M.M. Wilhelmus², Gertjan Veldhuis¹, Bart D. van Rooijen¹, Benjamin Drukarch², and Vinod Subramaniam¹

¹ Biophysical Engineering Group, MESA+ Institute for Nanotechnology and Institute for Biomedical Technology, University of Twente, 7500 AE Enschede, The Netherlands
² Department of Anatomy and Neurosciences, Institute for Clinical and Experimental Neurosciences (ICEN), VU University Medical Center, Amsterdam, The Netherlands

(RECEIVED April 29, 2008; FINAL REVISION May 22, 2008; ACCEPTED May 22, 2008)

We have studied the interaction of the enzyme tissue transglutaminase(tTG), catalyzing cross-link formation between protein-boundglutamine residues and primary amines, with Parkinson's disease-associated ${alpha}$ -synuclein protein variants at physiologically relevant concentrations.We have, for the first time, determined binding affinities oftTG for wild-type and mutant ${alpha}$ -synucleins using surface plasmonresonance approaches, revealing high-affinity nanomolar equilibriumdissociation constants. Nanomolar tTG concentrations were sufficientfor complete inhibition of fibrillization by effective ${alpha}$ -synucleincross-linking, resulting predominantly in intramolecularly cross-linkedmonomers accompanied by an oligomeric fraction. Since oligomericspecies have a pathophysiological relevance we further investigatedthe properties of the tTG/ ${alpha}$ -synuclein oligomers. Atomic forcemicroscopy revealed morphologically similar structures for oligomersfrom all ${alpha}$ -synuclein variants; the extent of oligomer formationwas found to correlate with tTG concentration. Unlike normal ${alpha}$ -synuclein oligomers the resultant structures were extremelystable and resistant to GdnHCl and SDS. In contrast to normalβ-sheet-containing oligomers, the tTG/ ${alpha}$ -synuclein oligomersappear to be unstructured and are unable to disrupt phospholipidvesicles. These data suggest that tTG binds equally effectiveto wild-type and disease mutant ${alpha}$ -synuclein variants. We proposethat tTG cross-linking imposes structural constraints on ${alpha}$ -synuclein,preventing the assembly of structured oligomers required fordisruption of membranes and for progression into fibrils. Ingeneral, cross-linking of amyloid forming proteins by tTG mayprevent the progression into pathogenic species.

Keywords: ${alpha}$ -synuclein; tissue transglutaminase; cross-linking; oligomer; surface plasmon resonance; atomic force microscopy; Parkinson's disease

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Tissue transglutaminase modulates -synuclein oligomerization

Tissue transglutaminase modulates ${alpha}$ -synuclein oligomerization