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dc.contributor.authorSerdaroglu, P
dc.contributor.authorMiddleton, L
dc.contributor.authorOhno, K
dc.contributor.authorChristodoulou, K
dc.contributor.authorBrengman, J
dc.contributor.authorMilone, M
dc.contributor.authorNeocleous, V
dc.contributor.authorDeymeer, F
dc.contributor.authorOzdemir, C
dc.contributor.authorMubaidin, A
dc.contributor.authorHorany, K
dc.contributor.authorAl-Shehab, A
dc.contributor.authorMavromatis, I
dc.contributor.authorMylonas, I
dc.contributor.authorTsingis, M
dc.contributor.authorZamba, E
dc.contributor.authorPantzaris, M
dc.contributor.authorKyriallis, K
dc.contributor.authorEngel, AG
dc.date.accessioned2021-03-03T11:56:20Z
dc.date.available2021-03-03T11:56:20Z
dc.date.issued1999
dc.identifier.citationMiddleton L., Ohno K., Christodoulou K., Brengman J., Milone M., Neocleous V., Serdaroglu P., Deymeer F., Ozdemir C., Mubaidin A., et al., "Chromosome 17p-linked myasthenias stem from defects in the acetylcholine receptor epsilon-subunit gene", NEUROLOGY, cilt.53, sa.5, ss.1076-1082, 1999
dc.identifier.issn0028-3878
dc.identifier.othervv_1032021
dc.identifier.otherav_2aeeb067-c936-4280-9e17-ba7c5795ae1e
dc.identifier.urihttp://hdl.handle.net/20.500.12627/33606
dc.identifier.urihttps://doi.org/10.1212/wnl.53.5.1076
dc.description.abstractObjective: To identify and to characterize functionally the mutational basis of congenital myasthenic syndromes (CMS) linked to chromosome 17p. Background: A total of 37 patients belonging to 13 CMS families, 9 of them consanguineous, were investigated. All patients were linked previously to the telomeric region of chromosome 17p. Two candidate genes in this region encode synaptobrevin 2, a presynaptic protein, and the epsilon-subunit of the acetylcholine receptor (AChR). Direct sequencing of the synaptobrevin 2 gene revealed no mutations. The authors thus searched for mutations in the epsilon-subunit gene of AChR. Methods: Direct sequencing of the AChR epsilon-subunit, restriction analysis, allele-specific PCR, and expression studies in human embryonic kidney cells were performed. Results: The authors identified two previously characterized and five novel epsilon-subunit gene mutations, all homozygous, in the 13 kinships. Two of the novel mutations are truncating (epsilon 723delC and epsilon 760ins8), one is a missense mutation in the signal peptide region (epsilon V-13D), one is a missense mutation in the N-terminal extracellular domain (epsilon T51P), and one is a splice donor site mutation in intron 10 (epsilon IVS10+2T-->G). Unaffected family members have no mutations or are heterozygous. Expression studies indicate that the four novel mutations in the coding region of the gene and the most likely transcript of the splice-site mutation, which skips exon 10, are low-expressor or null mutations. Conclusions: Chromosome 17p-linked congenital myasthenic syndromes are caused by low-expressor/null mutations in the AChR epsilon-subunit gene. Mutations in this gene are a common cause of CMS in eastern Mediterranean countries.
dc.language.isoeng
dc.subjectTıp
dc.subjectKlinik Tıp (MED)
dc.subjectKlinik Tıp
dc.subjectDahili Tıp Bilimleri
dc.subjectNöroloji
dc.subjectKLİNİK NEUROLOJİ
dc.subjectSağlık Bilimleri
dc.titleChromosome 17p-linked myasthenias stem from defects in the acetylcholine receptor epsilon-subunit gene
dc.typeMakale
dc.relation.journalNEUROLOGY
dc.contributor.department, ,
dc.identifier.volume53
dc.identifier.issue5
dc.identifier.startpage1076
dc.identifier.endpage1082
dc.contributor.firstauthorID123980


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