Heterogeneity in Four Families with MERRF Syndrome

Czech version

Authors: L. Stratilová; J. Zeman ¹; H. Houšťková; H. Hansíková; V. Konrádová; H. Hůlková ¹; M. Elleder ¹; E. Růžička ²; D. Tyl ²; E. Hrubá; J. Houštěk ³
Authors‘ workplace: Klinika dětského a dorostového lékařství 1. LF UK a VFN, Praha 1 Ústav dědičných poruch metabolismu 1. LF UK, Praha 2 Neurologická klinika 1. LF UK a VFN, Praha 3 Fyziologický ústav AV ČR, Praha
Published in: Čas. Lék. čes. 1999; : 401-405
Category:

Overview

Background.
The most frequent manifestation of mitochondrial DNA (mtDNA) mutation 8344 A ® G is MERRFsyndrome (Myoclonic Epilepsy and Myopathy with Ragged Red Fibres). Less frequent symptoms include ataxia,perceptive type of deafness, cardiomyopathy or external ophthalmoplegia and mental and motor retardation inchildren. We describe heterogeneity of clinical symptoms and results of biochemical and molecular investigationsin four families with the heteroplasmic mutation 8344 A ® G in mtDNA.Methods and Results. In co-operation with paediatric, neurological and genetic specialists from the Czech andSlovak Republic we found in 1993 - 1998 at the enzymatic or molecular level more than 90 children and adults withimpaired mitochondrial energy metabolism. Heteroplasmic mutation 8344 A ® G in mtDNA was found in fourfamilies. Ataxia and progressive muscle weakness appeared in the first proband with 50% of mutated copies ofmtDNA in muscle at the age of 30 years. The second proband with 95% of mutated mtDNA had his first clinicalsymptoms - muscle hypotonia, cardiomyopathy and mental and motor retardation - in infancy while his four relativeswith 25 - 50% mutated mtDNA lack so far clinical symptoms. In a female from the third family with 50% mutatedmtDNA in muscle the disease manifested at the age of 42 years with progressive external ophthalmoplegia (PEO)and muscle weakness. In the fourth proband with 50% of mutated mtDNA in blood the disease started in infancywith spastic quadruparesis and arrested mental and motor development. Enzymatic and histochemical investigationin muscle biopsy in two probands revealed lower cytochrom c oxidase activity. Ragged-red fibres were found onlyin one adult patient.Conclusions. MtDNA mutation 8344 A ® G can manifest by heterogeneous symptoms. A higher percentage ofmutated mtDNA is usually associated with more serious forms of the disease, but there is not always a correlationbetween the degree of heteroplasmy and severity of the disease or the age of the first clinical symptoms.

Key words:
MERRF syndrome, mtDNA, mutation 8344 A ® G, cytochrome c oxidase, clinical heterogeneity.

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Addictology Allergology and clinical immunology Angiology Audiology Clinical biochemistry Dermatology & STDs Paediatric gastroenterology Paediatric surgery Paediatric cardiology Paediatric neurology Paediatric ENT Paediatric psychiatry Paediatric rheumatology Diabetology Pharmacy Vascular surgery Pain management

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Article was published in

Journal of Czech Physicians

1999 Issue 13

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