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Genetic bases for glaucoma.

机译:青光眼的遗传基础。

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摘要

Glaucoma is the leading cause of visual impairment and blindness throughout the world. Primary open angle glaucoma (POAG; MIM 137760) is the main type of glaucoma in most populations, and more than 20 genetic loci for POAG have been reported. Only three causative genes have been identified in these loci, viz. myocilin (MYOC), optineurin (OPTN), and WD repeat domain 36 (WDR36). However, mutations in these genes account for only a small percentage of the patients with POAG. Some of these glaucoma cases have a Mendelian inheritance pattern, and a considerable fraction of the cases result from a large number of variants in several genes each contributing small effects. Glaucoma is considered to be a common disease such as diabetes mellitus, coronary disease, Crohn disease, and several( )common cancers. The main technological approaches used to identify the genes associated with glaucoma are the candidate gene approach, linkage analysis, case-control association study, and genome-wide association study. Association studies have found about 27 genes related to POAG, but the glaucoma-causing effects of these genes need to be investigated in more detail. The current trend is to use case-control association studies or genome-wide association studies to map the genes associated with glaucoma. Such studies are expected to greatly advance our understanding of the genetic basis of glaucoma, and to provide information on the effectiveness of glaucoma therapy. This review gives an overview on the genetic aspects of glaucoma.
机译:青光眼是全世界视力障碍和失明的主要原因。原发性开角型青光眼(POAG; MIM 137760)是大多数人群中的主要类型,据报道有20多个POAG基因位点。在这些基因座中,仅鉴定出三个致病基因。 myocilin(MYOC),optineurin(OPTN)和WD重复域36(WDR36)。但是,这些基因的突变仅占POAG患者的一小部分。这些青光眼病例中有一些具有孟德尔遗传模式,其中相当一部分病例是由几个基因中的大量变体导致的,每个变体的影响很小。青光眼被认为是一种常见疾病,例如糖尿病,冠状动脉疾病,克罗恩病和几种常见癌症。用于鉴定与青光眼相关的基因的主要技术方法是候选基因方法,连锁分析,病例对照关联研究和全基因组关联研究。协会研究发现了约27个与POAG相关的基因,但是这些基因引起青光眼的作用需要更详细地研究。当前的趋势是使用病例对照关联研究或全基因组关联研究来定位与青光眼有关的基因。这些研究有望极大地增进我们对青光眼遗传基础的理解,并提供有关青光眼治疗有效性的信息。这篇综述概述了青光眼的遗传方面。

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