一种伴有失明、肌张力障碍、骨折和智力缺陷的新的X连锁隐性耳聋综合征与Xq22相关。
A new X linked recessive deafness syndrome with blindness, dystonia, fractures, and mental deficiency is linked to Xq22.
作者信息
Tranebjaerg L, Schwartz C, Eriksen H, Andreasson S, Ponjavic V, Dahl A, Stevenson R E, May M, Arena F, Barker D
机构信息
Department of Medical Genetics, University Hospital, Tromsø, Norway.
出版信息
J Med Genet. 1995 Apr;32(4):257-63. doi: 10.1136/jmg.32.4.257.
X linked recessive deafness accounts for only 1.7% of all childhood deafness. Only a few of the at least 28 different X linked syndromes associated with hearing impairment have been characterised at the molecular level. In 1960, a large Norwegian family was reported with early onset progressive sensorineural deafness, which was indexed in McKusick as DFN-1, McKusick 304700. No associated symptoms were described at that time. This family has been restudied clinically. Extensive neurological, neurophysiological, neuroradiological, and biochemical, as well as molecular techniques, have been applied to characterise the X linked recessive syndrome. The family history and extensive characterisation of 16 affected males in five generations confirmed the X linked recessive inheritance and the postlingual progressive nature of the sensorineural deafness. Some obligate carrier females showed signs of minor neuropathy and mild hearing impairment. Restudy of the original DFN-1 family showed that the deafness is part of a progressive X linked recessive syndrome, which includes visual disability leading to cortical blindness, dystonia, fractures, and mental deficiency. Linkage analysis indicated that the gene was linked to locus DXS101 in Xq22 with a lod score of 5.37 (zero recombination). Based on lod-1 support interval of the multipoint analysis, the gene is located in a region spanning from 5 cM proximal to 3 cM distal to this locus. As the proteolipid protein gene (PLP) is within this region and mutations have been shown to be associated with non-classical PMD (Pelizaeus-Merzbacher disease), such as complex X linked hereditary spastic paraplegia, PLP may represent a candidate gene for this disorder. This family represents a new syndrome (Mohr-Tranebjaerg syndrome, MTS) and provides significant new information about a new X linked recessive sydromic type of deafness which was previously thought to be isolated deafness.
X连锁隐性聋仅占儿童期聋的1.7%。与听力障碍相关的至少28种不同的X连锁综合征中,只有少数在分子水平上得到了表征。1960年,报道了一个挪威大家庭,其成员患有早发性进行性感音神经性聋,在麦库西克氏人类遗传数据库中被编为DFN-1,麦库西克编号304700。当时未描述相关症状。对这个家庭进行了临床重新研究。广泛应用了神经学、神经生理学、神经放射学、生物化学以及分子技术来表征这种X连锁隐性综合征。对五代中16名受影响男性的家族史和广泛表征证实了X连锁隐性遗传以及感音神经性聋的语后进行性特征。一些肯定携带者女性表现出轻微神经病变和轻度听力障碍的迹象。对最初的DFN-1家庭的重新研究表明,耳聋是一种进行性X连锁隐性综合征的一部分,该综合征包括导致皮质盲的视力残疾、肌张力障碍、骨折和智力缺陷。连锁分析表明该基因与Xq22的DXS101位点连锁,优势对数得分为5.37(零重组)。基于多点分析的优势对数-1支持区间,该基因位于该位点近端5厘摩至远端3厘摩的区域内。由于蛋白脂质蛋白基因(PLP)在该区域内,且已表明突变与非典型佩利措伊斯-梅茨巴赫病(PMD)相关,如复杂的X连锁遗传性痉挛性截瘫,PLP可能是这种疾病的候选基因。这个家庭代表了一种新的综合征(莫尔-特拉内布尔格综合征,MTS),并提供了关于一种新的X连锁隐性综合征型耳聋的重要新信息,这种耳聋以前被认为是孤立性耳聋。
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