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Genetic linkage analyses and Cx50 mutation detection in a large multiplex Chinese family with hereditary nuclear cataract.

机译:遗传连锁白内障的一个庞大的多重中国家庭的遗传连锁分析和Cx50突变检测。

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摘要

PURPOSE: The aim of the study was to characterize the underlying mutation in a large multiplex Chinese family with hereditary nuclear cataract. METHODS: A 6-generation Chinese family having hereditary nuclear cataract was recruited and clinically verified. Blood DNA samples were obtained from 53 available family members. Linkage analyses were performed on the known candidate regions for hereditary cataract with 36 polymorphic microsatellite markers. To identify mutations related to cataract, a direct sequencing approach was applied to a candidate gene residing in our linkage locus. RESULTS: A linkage locus was identified with a maximum 2-point LOD score of 4.31 (recombination fraction = 0) at marker D1S498 and a maximum multipoint LOD score of 5.7 between markers D1S2344 and D1S498 on chromosome 1q21.1, where the candidate gene Cx50 is located. Direct sequencing of Cx50 showed a 139 G to A transition occurred in all affected family members. This transitional mutation resulted in a replacement of aspartic acid by asparagine at residue 47 (D47N) and led to a loss-of-function of the protein. CONCLUSIONS: The D47N mutation of Cx50 causes the hereditary nuclear cataract in this family in an autosomal dominant mode of inheritance with incomplete penetrance.
机译:目的:该研究的目的是鉴定一个遗传性白内障的大型多重中国家庭的潜在突变。方法:招募了具有遗传性白内障的6代中国家庭,并进行了临床验证。血液DNA样本获自53个可用的家庭成员。对遗传性白内障的已知候选区域进行了连锁分析,其中包括36种多态性微卫星标记。为了鉴定与白内障有关的突变,将直接测序方法应用于驻留在我们连锁基因座中的候选基因。结果:鉴定出一个连锁基因座,标记D1S498的最大2点LOD得分为4.31(重组分数= 0),而染色体1q21.1上的标记D1S2344和D1S498之间的最大多点LOD得分为5.7,其中候选基因Cx50位于。 Cx50的直接测序表明,在所有受影响的家庭成员中发生了139 G向A的转变。此过渡突变导致残基47(D47N)处的天冬酰胺替代天冬氨酸,并导致蛋白质功能丧失。结论:Cx50的D47N突变导致该家族的遗传性核性白内障以常染色体显性遗传,且外显率不完全。

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