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Phenotype of autosomal recessive congenital microphthalmia mapping to chromosome 14q32.

机译:常染色体隐性遗传性先天性小眼症的表型映射到染色体14q32。

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BACKGROUND: Congenital microphthalmia (OMIM: 309700) may occur in isolation or in association with a variety of systemic malformations. Isolated microphthalmia may be inherited as an autosomal dominant, an autosomal recessive, or an X linked trait. METHODS: Based on a whole genome linkage analysis, in a six generation consanguineous family with autosomal recessive inheritance, the first locus for isolated microphthalmia was mapped to chromosome 14q32. Eight members of this family underwent clinical examination to determine the nature of the microphthalmia phenotype associated with this locus. RESULTS: All affected individuals in this family suffered from bilateral microphthalmia in association with anterior segment abnormalities, and the best visual acuity achieved was "perception of light". Corneal changes included partial or complete congenital sclerocornea, and the later development of corneal vascularisation and anterior staphyloma. Intraocular pressure, as measured by Schiotz tonometry, was greatly elevated in many cases. CONCLUSIONS: This combination of ocular defects suggests an embryological disorder involving tissues derived from both the neuroectoderm and neural crest. Other families with defects in the microphthalmia gene located on 14q32 may have a similar ocular phenotype aiding their identification.
机译:背景:先天性小眼症(OMIM:309700)可能单独发生或与多种系统性畸形有关。孤立的小眼症可遗传为常染色体显性遗传,常染色体隐性遗传或X连锁性状。方法:基于全基因组连锁分析,在具有常染色体隐性遗传的六代近亲家族中,将分离出的小眼症的第一个基因座定位于染色体14q32。该家族的八名成员接受了临床检查,以确定与该基因座相关的小眼表型的性质。结果:该家族中所有受影响的个体均患有双侧小眼症并伴有前节异常,并且最佳视力为“光敏”。角膜变化包括部分或完全的先天性巩膜炎,以及后来的角膜血管化和前葡萄膜瘤发展。通过Schiotz眼压计测得的眼内压在许多情况下大大升高。结论:这种眼部缺陷的组合表明胚胎疾病涉及神经外胚层和神经c的组织。位于14q32上的小眼科基因中有缺陷的其他家族可能具有类似的眼表型,有助于其识别。

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