Kernhüllenerkrankungen - Eine neue Gruppe neuromuskulärer, kardiologischer und endokrinologischer Erkrankungen

F. Hanisch; S. Zierz

doi:10.1055/s-2003-42816

Aktuelle Neurologie 2003; 30(8): 369-374
DOI: 10.1055/s-2003-42816

Neues in der Neurologie

Kernhüllenerkrankungen - Eine neue Gruppe neuromuskulärer, kardiologischer und endokrinologischer Erkrankungen

Mutations of the Lamin A/C Protein as Cause for Neuromuscular, Cardiological and Endocrinological DiseasesF. Hanisch¹ , S. Zierz¹

¹Klinik und Poliklinik für Neurologie der Martin-Luther-Universität Halle-Wittenberg

Abstract

Zusammenfassung

Zurzeit sind zwei Kernhüllenproteine bekannt, das Lamin A/C und Emerin, bei denen Mutationen zu phänotypisch definierbaren Erkrankungen führen. Mutationen des auf dem Chromosom 1q21.2 - 1q21.3 kartierten LMNA-Gens bewirken Veränderungen der Proteine Lamin A und C. Die klinischen Manifestationsformen einer Mutation auf dem LMNA-Gen umfassen die Hauptmann-Thannhauser-Muskeldystrophie, die Gliedergürtelmuskeldystrophie 1B, die dilatative Kardiomyopathie 1A und die familiäre partielle Lipodystrophie Typ Dunnigan mit autosomal-dominantem Erbgang sowie die autosomal-rezessiv vererbte hereditäre sensomotorische Neuropathie Typ 2B (HSMN 2B). Die Erkrankungen mit autosomal-dominantem Erbgang zeigen nicht selten Phänotypen, deren Symptome sich überlappen können. Die Emery-Dreifuss-Muskeldystrophie mit X-chromosomalem Erbgang ist klinisch kaum von der Hauptmann-Thannhauser-Muskeldystrophie unterscheidbar. Molekulargenetisch liegt dieser Erkrankung jedoch eine Mutation des STA-Gens auf Chromosom Xq28 zugrunde, welches für Emerin, ein anderes Kernhüllenprotein, kodiert. Hinsichtlich der verschiedenen Mutationen im LMNA-Gen ist es bislang noch ungeklärt, wie Art und Lokalisation und eventuell modifizierende Faktoren den Phänotyp beeinflussen.

Abstract

There are two proteins of the nuclear envelope, lamin A/C and emerin, in which mutations are known to cause phenotypic distinguishable disorders. Mutations in the LMNA gene, mapped to chromosome 1q21.2 - 21.3, encoding nuclear proteins lamin A and C cause various disorders with autosomal-dominant inheritance. Some of these disorders show a phenotypical expression with overlapping symptoms as in Hauptmann-Thannhauser muscular dystrophy, limb girdle muscular dystrophy 1B, dilatative cardiomyopathy 1A, and rarely in the familial partiell lipodystrophy Typ Dunnigan, a metabolic disorder. Furthermore, mutations in the LMNA gene were recently found to cause the autosomal-recessive Charcot-Marie-Tooth disorder Type 2B (HSMN 2B) without muscular or metabolic involvement. The Xq28-linked Emery-Dreifuss muscular dystrophy due to mutations in the STA-gene encoding emerin is clinically not distinguishable from Hauptmann-Thannhauser muscular dystrophy. Concerning the different mutations it is an unsolved question how the kind and location as well as modifying factors are able to influence the phenotype.

Full Text

References

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Dr. med. F. Hanisch

Klinik und Poliklinik für Neurologie der Martin-Luther-Universität Halle-Wittenberg

Ernst-Grube-Straße 40

06097 Halle/Saale

Email: frank.hanisch@medizin.uni-halle.de