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Homozygosity mapping and linkage analysis demonstrate that autosomal recessive congenital hereditary endothelial dystrophy (CHED) and autosomal dominant CHED are genetically distinct

机译:纯合性作图和连锁分析表明常染色体隐性先天性遗传性血管内皮营养不良(CHED)和常染色体显性遗传性CHED在遗传上是不同的

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摘要

BACKGROUND—Congenital hereditary endothelial dystrophy (CHED) is a corneal dystrophy characterised by diffuse bilateral corneal clouding resulting in impaired vision. It is inherited in either an autosomal dominant (AD) or autosomal recessive (AR) manner. The AD form of CHED has been mapped to the pericentromeric region of chromosome 20. Another endothelial dystrophy, posterior polymorphous dystrophy (PPM), has been linked to a larger but overlapping region on chromosome 20. A large, Irish, consanguineous family with AR CHED was investigated to determine if there was linkage to this region.
METHODS—The technique of linkage analysis with polymorphic microsatellite markers amplified by polymerase chain reaction (PCR) was used. In addition, a DNA pooling approach to homozygosity mapping was employed to demonstrate the efficiency of this method.
RESULTS—Conventional genetic analysis in addition to a pooled DNA strategy excludes linkage of AR CHED to the AD CHED and larger PPMD loci.
CONCLUSION—This demonstrates that AR CHED is genetically distinct from AD CHED and PPMD.

 Keywords: congenital hereditary endothelial dystrophy; homozygosity mapping; posterior polymorphous dystrophy; linkage analysis
机译:背景—先天性遗传性内皮营养不良(CHED)是一种角膜营养不良,其特征是弥漫性双侧角膜混浊导致视力受损。它以常染色体显性(AD)或常染色体隐性(AR)方式遗传。 CHED的AD形式已定位到20号染色体的着丝粒区域。另一种内皮营养不良,后多态性营养不良(PPM)与20号染色体上较大但重叠的区域有关.AR CHED的爱尔兰近亲大家族被调查以确定是否与该区域有联系。方法—使用通过聚合酶链反应(PCR)扩增的多态微卫星标记进行连锁分析的技术。此外,采用DNA池纯合性作图方法证明了该方法的有效性。结果—除了常规DNA分析之外,常规遗传分析还排除了AR CHED与AD CHED和更大的PPMD基因座的联系。结论—这表明AR CHED在遗传上不同于AD CHED和PPMD。关键词:先天性遗传性血管营养不良;纯合性作图;后部多态性营养不良连锁分析

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