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Novel mutations in CACNA1F and NYX in Dutch families with X-linked congenital stationary night blindness.

机译:X连锁先天性固定性夜盲的荷兰家庭中CACNA1F和NYX的新型突变。

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摘要

PURPOSE: To describe the clinical features and genetic analysis of eight X-linked congenital stationary night blindness (XLCSNB) Dutch patients. METHODS: Electroretinogram (ERG) measurements were assessed in Dutch patients. Molecular genetic testing by denaturing high performance liquid chromatography (DHPLC), single stranded conformation polymorphism (SSCP) analysis, and direct sequencing of the CACNA1F and NYX genes were performed in the patients possessing a negative Schubert Bornschein ERG. RESULTS: Molecular genetic testing of CACNA1F and NYX revealed three novel and two known CACNA1F sequence variants as well as two novel sequence alterations in the NYX gene. While one of the CACNA1F sequence variants (5756G>A, R1919H) has been previously described as a common polymorphism in Japanese families, we did not found this transition in 100 European control alleles. CONCLUSIONS: In a pool of eight diagnosed XLCSNB patients, five showed a sequence variation in the CACNA1F and two in the NYX gene. In only one of the eight patients no sequence alteration could be detected. This might be explained by a mutation in other, as yet unidentified coding or regulatory sequences of NYX or CACNA1F or additional genes.
机译:目的:描述8名X连锁先天性固定性夜盲症(XLCSNB)荷兰患者的临床特征和遗传分析。方法:对荷兰患者进行了视网膜电图(ERG)测量。 Schubert Bornschein ERG阴性的患者通过变性高效液相色谱(DHPLC),单链构象多态性(SSCP)分析以及CACNA1F和NYX基因的直接测序进行分子遗传学测试。结果:CACNA1F和NYX的分子遗传学测试揭示了三个新的和两个已知的CACNA1F序列变体,以及NYX基因中的两个新的序列改变。虽然先前已将CACNA1F序列变异之一(5756G> A,R1919H)描述为日本家族中的常见多态性,但我们并未在100个欧洲对照等位基因中发现这种转变。结论:在八名被诊断为XLCSNB的患者中,五名在CACNA1F中表现出序列变异,而两名在NYX基因中表现出序列变异。在八名患者中只有一名无法检测到序列改变。这可能是由于NYX或CACNA1F或其他基因的其他尚未确定的编码或调控序列突变引起的。

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