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后极性白内障是PITX3基因反复突变的主要后果。

Posterior polar cataract is the predominant consequence of a recurrent mutation in the PITX3 gene.

作者信息

Addison P K F, Berry V, Ionides A C W, Francis P J, Bhattacharya S S, Moore A T

机构信息

Department of Molecular Genetics, Institute of Ophthalmology, London, UK.

出版信息

Br J Ophthalmol. 2005 Feb;89(2):138-41. doi: 10.1136/bjo.2004.053413.

DOI:10.1136/bjo.2004.053413
PMID:15665340
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1772502/
Abstract

BACKGROUND

The authors recently identified three large genetically unrelated families with an identical 17 base pair duplication mutation in exon 4 of the PITX3 gene. Here, they report the detailed clinical phenotype.

METHODS

Affected and unaffected individuals in the three families with autosomal dominant posterior polar cataract underwent full clinical examination and donated blood samples for DNA extraction and molecular genetic studies.

RESULTS

In all three families, an identical 17 base pair duplication mutation in PITX3 was identified which co-segregated with disease status in the family. All affected individuals had bilateral progressive posterior polar cataracts. In one family, posterior polar cataract was the only clinical abnormality but in the other two families, one of 10 affected individuals and four of 11 affected individuals also had anterior segment mesenchymal dysgenesis (ASMD).

CONCLUSION

Mutations in the PITX3 gene in humans result in posterior polar cataract and variable ASMD. The gene encodes a transcription factor which has a key role in lens and anterior segment development. The mechanism by which the mutant protein gives rise to such a regional pattern of lens opacity remains to be elucidated.

摘要

背景

作者最近在三个无亲缘关系的大家族中发现,PITX3基因外显子4存在相同的17个碱基对重复突变。在此,他们报告详细的临床表型。

方法

对这三个常染色体显性遗传后极性白内障家族中的患病个体和未患病个体进行全面临床检查,并采集血样用于DNA提取和分子遗传学研究。

结果

在所有三个家族中均发现PITX3基因存在相同的17个碱基对重复突变,且该突变与家族中的疾病状态共分离。所有患病个体均患有双侧进行性后极性白内障。在一个家族中,后极性白内障是唯一的临床异常,但在另外两个家族中,10名患病个体中的1名以及11名患病个体中的4名还患有前段间充质发育异常(ASMD)。

结论

人类PITX3基因突变会导致后极性白内障和可变的ASMD。该基因编码一种转录因子,其在晶状体和前段发育中起关键作用。突变蛋白导致晶状体混浊呈现这种区域模式的机制仍有待阐明。

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