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Novel mutations of mitochondrial complex I in pathologically proven Parkinson disease
Authors:Siegfried Kösel  E. M. Grasbon-Frodl  Ulrike Mautsch  Rupert Egensperger  U. von Eitzen  Dimitrij Frishman  Sabine Hofmann  Klaus-Dieter Gerbitz  Parviz Mehraein  Manuel B. Graeber
Affiliation:Molecular Neuropathology Laboratory, Institute of Neuropathology, Ludwig-Maximilians-University, Munich, Germany.
Abstract:Complete sequence analysis of all mitochondrial complex I genes was performed in 22 cases of neuropathologically confirmed idiopathic Parkinson disease (PD). DNA from the substantia nigra was used as a template for polymerase chain reaction-based genomic sequencing. Seven novel mutations causing the exchange of amino acids were detected in subunit genes ND1 (3992 C/T, 4024 A/G), ND4 (11253 T/C, 12084 C/T), ND5 (13711 G/A, 13768 T/C), and ND6 (14582 T/C). In addition, five known missense mutations affecting the ND1 (3335 T/C, 3338 T/C), ND2 (5460 G/A), ND3 (10398 A/G), and ND5 (13966 A/G) genes as well as three secondary LHON mutations (4216 T/C, 4917 A/G, 13708 G/A) were found in the PD group. Among the novel mutations, the 11253 T/C transition which changes a conserved isoleucine residue into threonine is most likely to be of functional relevance. Furthermore, 43 synonymous polymorphisms were detected in PD brains, including 20 novel sequence variants. Haplogroup analysis revealed that most unique missense mutations were found in PD cases belonging to the Dc haplogroup. Our data are in line with the view that PD is not a single disease entity but comprises a genetically heterogeneous group of disorders. The results of our study further suggest that 90% or more of all idiopathic PD cases are not due to sequence variation of mitochondrial complex I, but that mitochondrial mutations may play a pathogenic role in a subset of PD patients. Received: November 24, 1997 / Accepted: December 18, 1997
Keywords:  Genetic heterogeneity  Mitochondrial haplogroups  NADH dehydrogenase  Susceptibility genes
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