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首页> 外文期刊>Human Genetics >The mutation spectrum of the bestrophin protein--functional implications.
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The mutation spectrum of the bestrophin protein--functional implications.

机译:Bestrophin蛋白的突变谱-功能含义。

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Best's macular dystrophy (BMD), also known as vitelliform macular degeneration type 2 (VMD2; OMIM 153700), is an autosomal dominant form of macular degeneration with mainly juvenile onset. BMD is characterized by the accumulation of lipofuscin within and beneath the retinal pigment epithelium. The gene causing the disease has been localized to 11q13 by recombination breakpoint mapping. Recently, we have identified the causative gene encoding a protein named bestrophin, and mutations have been found mainly to affect residues that are conserved from a family of genes in Caenorhabditis elegans. The function of bestrophin is so far unknown, and no reliable predictions can be made from sequence comparisons. We have investigated the bestrophin gene in 14 unrelated Swedish, Dutch, Danish, and Moroccan families affected with BMD and found eight new mutations. Including the previously published mutations, 15 different missense mutations have now been detected in 19 of the 22 families with BMD investigated by our laboratory. Interestingly, the mutations cluster in certain regions, and no nonsense mutations or mutations causing frame-shifts have been identified. Computer simulations of the structural elements in the bestrophin protein show that this protein is probably membrane bound, with four putative transmembrane regions.
机译:Best的黄斑营养不良(BMD),也称为2型玻璃样黄斑变性(VMD2; OMIM 153700),是一种以黄体变性为主的常染色体显性形式,主要发病于青少年。 BMD的特征是脂褐素在视网膜色素上皮内和下方积聚。通过重组断点定位,导致该疾病的基因已定位于11q13。最近,我们已经鉴定出编码一种名为Bestrophin的蛋白质的致病基因,并且发现突变主要影响秀丽隐杆线虫中一个基因家族的保守残基。迄今为止,Bestrophin的功能尚不清楚,无法通过序列比较做出可靠的预测。我们已经调查了14个无关的瑞典,荷兰,丹麦和摩洛哥受BMD感染的家庭中的Bestrophin基因,发现了8个新突变。包括先前公布的突变在内,我们实验室在22个BMD家庭中的19个家庭中现已检测到15个不同的错义突变。有趣的是,突变聚集在某些区域,并且尚未鉴定出无意义的突变或引起移码的突变。 Bestrophin蛋白中结构元素的计算机模拟表明,该蛋白可能与膜结合,具有四个假定的跨膜区域。

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