1. A human neuronal tissue culture model for Lesch-Nyhan disease
- Author
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Alokes Majumdar, Irène Ceballos-Picot, Mairead Kelly, Kiyoshi Egami, Thomas L. Shirley, Hyder A. Jinnah, J. Chris Lewers, and Michael M. Seidman
- Subjects
Purine ,Biology ,medicine.disease ,Xanthine ,Biochemistry ,Molecular biology ,Cellular and Molecular Neuroscience ,chemistry.chemical_compound ,chemistry ,Hypoxanthine-guanine phosphoribosyltransferase ,Adenine nucleotide ,medicine ,Lesch–Nyhan syndrome ,Purine metabolism ,Hypoxanthine ,Hypoxanthine Phosphoribosyltransferase - Abstract
Mutations in the gene encoding the purine salvage enzyme, hypoxanthine-guanine phosphoribosyltransferase (HPRT) cause Lesch-Nyhan disease, a neurodevelopmental disorder characterized by cognitive, neurological, and behavioral abnormalities. Despite detailed knowledge of the enzyme's function, the key pathophysiological changes that accompany loss of purine recycling are unclear. To facilitate delineating the consequences of HPRT deficiency, four independent HPRT-deficient sublines of the human dopaminergic neuroblastoma, SK-N-BE(2) M17, were isolated by targeted mutagenesis with triple helix-forming oligonucleotides. As a group, these HPRT-deficient cells showed several significant abnormalities: (i) impaired purine recycling with accumulation of hypoxanthine, guanine, and xanthine, (ii) reduced guanylate energy charge and GTP:GDP ratio, but normal adenylate energy charge and no changes in any adenine nucleotide ratios, (iii) increased levels of UTP and NADP+, (iv) reduced DOPA decarboxylase, but normal monoamines, and (v) reduction in cell soma size. These cells combine the analytical power of multiple lines and a human, neuronal origin to provide an important tool to investigate the pathophysiology of HPRT deficiency.
- Published
- 2007
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