MELAS: a new disease associated mitochondrial DNA mutation and evidence for further genetic heterogeneity

OBJECTIVES To define the molecular genetic basis of the MELAS phenotype in five patients without any known mutation of mitochondrial DNA. METHODS Systematic automated mitochondrial DNA sequencing of all mitochondrial transfer RNA and cytochrome c oxidase genes was undertaken in five patients who had...

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Bibliographic Details
Published in:Journal of neurology, neurosurgery and psychiatry neurosurgery and psychiatry, 1998-10, Vol.65 (4), p.512-517
Main Authors: Hanna, M G, Nelson, I P, Morgan-Hughes, J A, Wood, N W
Format: Article
Language:English
Subjects:
Adult
Age
Ataxia
Atrophy
Biological and medical sciences
Biopsy
Convulsions & seizures
Diseases of striated muscles. Neuromuscular diseases
DNA Primers - genetics
DNA, Mitochondrial - genetics
Eye movements
Family medical history
Female
Headaches
Humans
Male
Medical sciences
MELAS
MELAS Syndrome - diagnosis
MELAS Syndrome - genetics
Middle Aged
Mitochondrial DNA
Mutation
Nausea
Neurology
Patients
Phenotype
Phenylalanine - genetics
Plasma
Point Mutation - genetics
Polymerase Chain Reaction - methods
RNA, Transfer, Amino Acid-Specific - genetics
Stroke
Transfer RNA
tRNA gene
Vomiting
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Summary:OBJECTIVES To define the molecular genetic basis of the MELAS phenotype in five patients without any known mutation of mitochondrial DNA. METHODS Systematic automated mitochondrial DNA sequencing of all mitochondrial transfer RNA and cytochrome c oxidase genes was undertaken in five patients who had the MELAS phenotype. RESULTS A novel heteroplasmic mitochondrial DNA mutation was identified in the transfer RNA gene for phenylalanine in one case (patient 3). This mutation was not detected in the patient’s blood or in her mother’s blood. No pathogenic mutations were identified in the other four patients. CONCLUSIONS This is the first point mutation in the transfer RNA gene for phenylalanine to be associated with MELAS. The absence of mutations in the remaining four patients suggests that there is further genetic heterogeneity associated with this mitochondrial phenotype.
ISSN:0022-3050
1468-330X
DOI:10.1136/jnnp.65.4.512