The phenotypic spectrum of fifty Czech m.3243A>G carriers

Mitochondrial myopathy, Encephalopathy, Lactic Acidosis and Stroke-like episodes syndrome (MELAS) is a common mitochondrial disorder with varying multisystemic clinical manifestation. We present a comprehensive clinical picture of 50 Czech m.3243A>G carriers with emphasis on the sequence of sympt...

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Bibliographic Details
Published in:Molecular genetics and metabolism 2016-08, Vol.118 (4), p.288-295
Main Authors: Dvorakova, V., Kolarova, H., Magner, M., Tesarova, M., Hansikova, H., Zeman, J., Honzik, T.
Format: Article
Language:English
Subjects:
Adolescent
Adult
Child
Child, Preschool
Czech Republic
DNA, Mitochondrial - genetics
Female
Fully expressed phenotype
Heteroplasmy
Heterozygote
Humans
Infant
m.3243A > G
Male
MELAS
MELAS Syndrome - genetics
MELAS Syndrome - mortality
MELAS Syndrome - physiopathology
Middle Aged
Mitochondrial Myopathies - genetics
Mitochondrial Myopathies - mortality
Mitochondrial Myopathies - physiopathology
Mutation
Natural course
Oligosymptomatic patients
Phenotype
RNA, Transfer, Leu - genetics
Young Adult
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Summary:Mitochondrial myopathy, Encephalopathy, Lactic Acidosis and Stroke-like episodes syndrome (MELAS) is a common mitochondrial disorder with varying multisystemic clinical manifestation. We present a comprehensive clinical picture of 50 Czech m.3243A>G carriers with emphasis on the sequence of symptoms in symptomatic patients. Symptoms developed in 33 patients (66%) and 17 carriers remained unaffected (34%). The age of onset varied from 1month to 47years of age, with juvenile presentation occurring in 53% of patients. Myopathy was the most common presenting symptom (18%), followed by CPEO/ptosis and hearing loss, with the latter also being the most common second symptom. Stroke-like episodes (SLE) occurred in fourteen patients, although never as a first symptom, and were frequently preceded by migraines (58%). Rhabdomyolysis developed in two patients. The second symptom appeared 5.0±8.3years (range 0–28years) after the first, and the interval between the second and third symptom was 2.0±6.0years (range 0–21years). Four of our patients remained monosymptomatic up to 12years of follow-up. The sequence of symptoms according to their time of manifestation was migraines, myopathy, seizures, CPEO/ptosis, SLE, hearing loss, and diabetes mellitus. The average age at death was 32.4±17.7years (range 9–60years) in the juvenile form and 44.0±12.7years (range 35–53years) in the adult form. Some patients with SLE harboured very low heteroplasmy levels in various tissues. No threshold for any organ dysfunction could be determined based on these levels. Sufficient knowledge of the timeline of the natural course of MELAS syndrome may improve the prediction and management of symptoms in patients with this mitochondrial disease. •Myopathy is the most common presenting symptom and rhabdomyolysis may develop.•Stroke-like episodes always ensue other symptoms and in 58% are preceded by migraines.•Any symptom of MELAS may come first and intersymptom interval may reach up to 28years.•Juvenile form has a higher mortality rate than adult form of the disease.•Even mono and oligosymptomatic patients should be taken into consideration for MELAS.
ISSN:1096-7192
1096-7206
DOI:10.1016/j.ymgme.2016.06.003