Synthesis, physicochemical characterization and neuroprotective evaluation of novel 1-hydroxypyrazin-2(1H)-one iron chelators in an in vitro cell model of Parkinson's disease

Frank W. Lewis; Kathleen Bird; Jean-Philippe Navarro; Rawa El Fallah; Jeremy Brandel; Véronique Hubscher-Bruder; Andrew Tsatsanis; James A. Duce; David Tétard; Samuel Bourne; Mahmoud Maina; Ilse S. Pienaar

doi:10.1039/D1DT02604F

Synthesis, physicochemical characterization and neuroprotective evaluation of novel 1-hydroxypyrazin-2(1H)-one iron chelators in an in vitro cell model of Parkinson's disease†

Frank W. Lewis,

*^a Kathleen Bird,^a Jean-Philippe Navarro,^a Rawa El Fallah,^b Jeremy Brandel,^b Véronique Hubscher-Bruder,

^b Andrew Tsatsanis,^cd James A. Duce,^cd David Tétard,

^a Samuel Bourne,^e Mahmoud Maina^e and Ilse S. Pienaar

^ef

Author affiliations

* Corresponding authors

^a Department of Applied Sciences, Faculty of Health and Life Sciences, Northumbria University, Newcastle upon Tyne, Tyne and Wear NE1 8ST, UK
E-mail: frank.lewis@northumbria.ac.uk
Fax: +44 (0)0191 227 3519
Tel: +44 (0)191 227 4637

^b Université de Strasbourg, CNRS, IPHC UMR 7178, F-67000 Strasbourg, France
E-mail: jbrandel@unistra.fr
Tel: +33 (0)368 852 749

^c School of Biomedical Sciences, The Faculty of Biological Sciences, University of Leeds, Leeds, West Yorkshire LS2 9JT, UK

^d Alzheimer's Research UK Cambridge Drug Discovery Institute, Cambridge Bio-medical Campus, University of Cambridge, Cambridge, UK
E-mail: jad205@cam.ac.uk
Tel: +44 (0)1223 335 656

^e School of Life Sciences, University of Sussex, Falmer, Sussex BN1 9PH, UK
E-mail: I.S.Pienaar@sussex.ac.uk
Tel: +44 (0)1273 678 057

^f Institute of Clinical Sciences, University of Birmingham, Edgbaston, Birmingham B15 2TT, UK

Abstract

Iron dysregulation, dopamine depletion, cellular oxidative stress and α-synuclein protein mis-folding are key neuronal pathological features seen in the progression of Parkinson's disease. Iron chelators endowed with one or more therapeutic modes of action have long been suggested as disease modifying therapies for its treatment. In this study, novel 1-hydroxypyrazin-2(1H)-one iron chelators were synthesized and their physicochemical properties, iron chelation abilities, antioxidant capacities and neuroprotective effects in a cell culture model of Parkinson's disease were evaluated. Physicochemical properties (log β, log D_7.4, pL_0.5) suggest that these ligands have a poorer ability to penetrate cell membranes and form weaker iron complexes than the closely related 1-hydroxypyridin-2(1H)-ones. Despite this, we show that levels of neuroprotection provided by these ligands against the catecholaminergic neurotoxin 6-hydroxydopamine in vitro were comparable to those seen previously with the 1-hydroxypyridin-2(1H)-ones and the clinically used iron chelator Deferiprone, with two of the ligands restoring cell viability to ≥89% compared to controls. Two of the ligands were endowed with additional phenol moieties in an attempt to derive multifunctional chelators with dual iron chelation/antioxidant activity. However, levels of neuroprotection with these ligands were no greater than ligands lacking this moiety, suggesting the neuroprotective properties of these ligands are due primarily to chelation and passivation of intracellular labile iron, preventing the generation of free radicals and reactive oxygen species that otherwise lead to the neuronal cell death seen in Parkinson's disease.

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Synthesis, physicochemical characterization and neuroprotective evaluation of novel 1-hydroxypyrazin-2(1H)-one iron chelators in an in vitro cell model of Parkinson's disease†

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Synthesis, physicochemical characterization and neuroprotective evaluation of novel 1-hydroxypyrazin-2(1H)-one iron chelators in an in vitro cell model of Parkinson's disease

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