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Evidence for a novel glaucoma locus at chromosome 3p21-22.

机译:染色体3p21-22处有新的青光眼基因座的证据。

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摘要

Primary open-angle glaucoma (POAG) is one of the leading causes of blindness in the world. It is a clinically variable group of diseases with the majority of cases presenting as the late onset adult type. Several chromosomal loci have been implicated in disease aetiology, but causal mutations have only been identified in a small proportion of glaucoma. We have previously described a large six-generation Tasmanian family with POAG exhibiting genetic heterogeneity. In this family, approximately one third of affected individuals presented with a glutamine-368-STOP (Q368STOP) mutation in the myocilin gene. We now use a Markov Chain Monte Carlo (MCMC) method to identify a second disease region in this family on the short arm of chromosome 3. This disease locus was initially mapped to the marker D3S1298 and a subsequent minimum disease region of 9 cM between markers D3S1298 and D3S1289 was identified through additional mapping. The region did not overlap with any previously described locus for POAG. Using a multiplicative relative risk model, we identified a positive association between this region and the Q368STOP mutation of myocilin on chromosome 1 in affected individuals. These findings provide evidence of a new autosomal dominant glaucoma locus on the short arm of chromosome 3.
机译:原发性开角型青光眼(POAG)是世界上导致失明的主要原因之一。它是临床上可变的一组疾病,大多数病例为成年晚期成年人。几个染色体位点已与疾病病因有关,但仅在一小部分青光眼中发现了因果突变。我们之前已经描述了一个大型的塔斯马尼亚六世家族,其POAG表现出遗传异质性。在这个家庭中,大约三分之一的受影响个体在myocilin基因中出现了谷氨酰胺-368-STOP(Q368STOP)突变。现在,我们使用马尔可夫链蒙特卡罗(MCMC)方法在3号染色体短臂上鉴定该家族中的第二个疾病区域。该疾病基因座最初被定位到标记D3S1298,随后两个标记之间的最小疾病区域为9 cM。 D3S1298和D3S1289是通过其他映射确定的。该区域与任何先前描述的POAG基因座均不重叠。使用乘法相对风险模型,我们确定了该区域与患病个体1号染色体上的myocilin Q368STOP突变之间呈正相关。这些发现提供了3号染色体短臂上新的常染色体显性青光眼基因座的证据。

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