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Genetics of primary open angle glaucoma

机译:原发性开角型青光眼的遗传学

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Glaucoma is a neurodegenerative disease and one of the leading causes of irreversible blindness, affecting over 60 million people worldwide. At the present time, glaucoma is clinically defined, but the exact etiology is unknown. Genetic studies are one approach to identify the molecules and pathways involved in disease pathogenesis. Familial aggregation of primary open-angle glaucoma (POAG) has long been recognized, and the analysis of POAG families with a Mendelian inheritance form of this disease has been employed to identify multiple loci linked to them. Some causative genes, such as myocilin, optineurin and WD repeat domain 36, have been identified. However, most cases of POAG are considered to be a prevalent, multifactorial disorder. Several association studies have been conducted for candidate genes, and genome-wide association studies recently identified new susceptibility loci for POAG, namely, S1 RNA binding domain 1 region on chromosome 2p21, the caveolin 1 and caveolin 2 regions on 7q31, transmembrane and coiled-coil domain 1 region on 1q24, cyclin-dependent kinase inhibitor 2B antisense RNA on 9p21, the SIX1 and SIX6 regions on 14q24 and, possibly, the regulatory region of 8q22. Further analysis of clinical manifestations caused by specific genes and functional analysis of these genes will contribute to the development of new strategies for the diagnosis and treatment of POAG.
机译:青光眼是一种神经退行性疾病,是不可逆性失明的主要原因之一,在全球范围内影响了超过6000万人。目前,临床上已定义了青光眼,但确切的病因尚不清楚。遗传研究是鉴定涉及疾病发病机制的分子和途径的一种方法。家族性聚集的原发性开角型青光眼(POAG)早已得到认可,对具有该疾病孟德尔遗传形式的POAG家族的分析已用于鉴定与其相关的多个基因座。某些致病基因,如myocilin,optineurin和WD重复结构域36,已被鉴定。但是,大多数POAG病例被认为是一种普遍的多因素疾病。已针对候选基因进行了几项关联研究,最近全基因组关联研究确定了POAG的新易感性基因座,即染色体2p21上的S1 RNA结合结构域1区,7q31上的小窝蛋白1和小窝蛋白2区,跨膜和卷曲螺旋。 1q24上的卷曲结构域1区,9p21上的细胞周期蛋白依赖性激酶抑制剂2B反义RNA,14q24上的SIX1和SIX6区以及可能的8q22调控区。由特定基因引起的临床表现的进一步分析和这些基因的功能分析将有助于开发诊断和治疗POAG的新策略。

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