一个常染色体显性遗传性青少年型青光眼家族的临床特征及连锁分析

Clinical features and linkage analysis of a family with autosomal dominant juvenile glaucoma.

作者信息

Johnson A T, Drack A V, Kwitek A E, Cannon R L, Stone E M, Alward W L

机构信息

University of Iowa Hospitals and Clinics, Iowa City 52242.

出版信息

Ophthalmology. 1993 Apr;100(4):524-9. doi: 10.1016/s0161-6420(13)31615-7.

DOI:10.1016/s0161-6420(13)31615-7

PMID:8479711

Abstract

BACKGROUND

Juvenile glaucoma is an uncommon form of open-angle glaucoma that is usually recognized during childhood or early adulthood and which often has a strong family history.

METHODS

The authors clinically characterized a large multigeneration family with autosomal-dominant, juvenile-onset, open-angle glaucoma. Linkage analysis with short tandem repeat polymorphisms was used to evaluate the Rieger's syndrome locus as the site of the disease-causing mutation.

RESULTS

Forty members of a family with a five-generation history of open-angle glaucoma were examined. Clinical data were available from an additional five individuals, three of whom were decreased. Older family members provided limited information about the visual history of five other deceased individuals in the first three generations. Fifty-nine people were at 50% risk of harboring the disease-causing mutation; and of these, 30 were affected with glaucoma by examination or by family history. All affected patients had an affected parent. The average age at diagnosis was 18 years (range, 8-30 years). Affected family members tended to be myopic but lacked other ocular or systemic abnormalities. The intraocular pressures (IOPs) of affected individuals were commonly more than 50 mmHg when they were first examined. Gonioscopy showed the angles to be open, with no abnormal pigmentation, iris processes, or embryonic tissue. Topical medications were initially effective in controlling IOP, but surgery was usually required for long-term pressure control. The Rieger's syndrome locus on chromosome 4q25 was excluded as the site of the disease-causing mutation.

CONCLUSION

Juvenile open-angle glaucoma can occur as an autosomal dominant trait with high penetrance. Genetic linkage analysis of the family reported here has the potential to identify the chromosomal location of a glaucoma-causing gene. This gene is genetically distinct from the chromosome 4 locus that was recently associated with Rieger's syndrome.

摘要

背景

青少年青光眼是开角型青光眼的一种罕见形式，通常在儿童期或成年早期被发现，且往往有很强的家族病史。

方法

作者对一个常染色体显性遗传、青少年发病的开角型青光眼的大型多代家族进行了临床特征分析。使用短串联重复多态性进行连锁分析，以评估里格尔综合征基因座作为致病突变的位点。

结果

对一个有五代开角型青光眼病史的家族中的40名成员进行了检查。另外5名个体有临床数据，其中3名视力下降。年长的家族成员提供了关于前三代中另外5名已故个体视觉病史的有限信息。59人有50%的风险携带致病突变；其中，30人经检查或家族病史诊断患有青光眼。所有患病患者均有患病的父母。诊断时的平均年龄为18岁（范围8 - 30岁）。患病家族成员往往近视，但无其他眼部或全身异常。首次检查时，患病个体的眼压通常超过50 mmHg。前房角镜检查显示房角开放，无异常色素沉着、虹膜突或胚胎组织。局部用药最初对控制眼压有效，但长期眼压控制通常需要手术。位于4q25染色体上的里格尔综合征基因座被排除为致病突变位点。