高加索人群中肌纤蛋白Gly252Arg突变与中度青光眼

Myocilin Gly252Arg mutation and glaucoma of intermediate severity in Caucasian individuals.

作者信息

Hewitt Alex W, Bennett Sonya L, Richards Julia E, Dimasi David P, Booth Adam P, Inglehearn Chris, Anwar Rashida, Yamamoto Tetsuya, Fingert John H, Héon Elise, Craig Jamie E, Mackey David A

机构信息

Clinical Genetics Unit, Eye Research Australia, University of Melbourne, Royal Victorian Eye & Ear Hospital, Melbourne, Australia.

出版信息

Arch Ophthalmol. 2007 Jan;125(1):98-104. doi: 10.1001/archopht.125.1.98.

DOI:10.1001/archopht.125.1.98

PMID:17210859

Abstract

OBJECTIVE

To determine the phenotype of an Australian pedigree with the myocilin (MYOC) Gly252Arg mutation, comparing it with other pedigrees carrying the same mutation.

METHODS

All recruited subjects underwent a comprehensive clinical examination, including optic disc assessment, applanation tonometry, and visual field measurement. Mutation analysis was performed through direct sequencing. Haplotype analysis was performed using microsatellite markers around the MYOC gene.

RESULTS

Eight Gly252Arg mutation carriers with glaucoma were identified from the same pedigree. Carriers' mean +/- SD age at diagnosis was 46.3 +/- 11.4 years (range, 31-60 years). Highest recorded intraocular pressure ranged from 27 to 42 mm Hg (mean +/- SD, 32.4 +/- 5.6 mm Hg). Cup-disc ratios in the worst eye ranged from 0.6 to 0.9. Six of the 8 individuals had undergone filtration surgery. A common founding haplotype between MY5 and D1S218 was found for Caucasian individuals tested with this mutation. One subject was compound heterozygotic for the MYOC Gly252Arg mutation and a novel MYOC Gly244Val variant.

CONCLUSIONS

Although a common founder for Gly252Arg across Caucasian subjects was found, the phenotype from this Australian MYOC mutation-carrying pedigree is less severe than previously described. The severity of glaucoma caused by the Gly252Arg mutation may be similar to the Thr377Met MYOC mutation, yet is more severe than the most common Gln368Stop mutation.

CLINICAL RELEVANCE

Since its implication in glaucoma, much work has been performed investigating the clinical features of MYOC-related glaucoma. Given the strong genotype-phenotype correlations with MYOC disease-causing variants, health care professionals armed with such molecular information are able to accurately counsel patients on their likely disease course. Our work suggests that the disease associated with MYOC Gly252Arg is less severe than previously described in other pedigrees with this specific mutation.

摘要

目的

确定一个携带肌纤蛋白（MYOC）Gly252Arg突变的澳大利亚家系的表型，并与其他携带相同突变的家系进行比较。

方法

所有招募的受试者均接受了全面的临床检查，包括视盘评估、压平眼压测量和视野测量。通过直接测序进行突变分析。使用MYOC基因周围的微卫星标记进行单倍型分析。

结果

从同一个家系中鉴定出8名携带Gly252Arg突变且患有青光眼的患者。携带者诊断时的平均年龄±标准差为46.3±11.4岁（范围为31 - 60岁）。记录到的最高眼压范围为27至42毫米汞柱（平均±标准差，32.4±5.6毫米汞柱）。最差眼睛的杯盘比范围为0.6至0.9。8名个体中有6人接受了滤过手术。对于检测到该突变的白种人个体，发现MY5和D1S218之间存在一个共同的始祖单倍型。一名受试者为MYOC Gly252Arg突变和一种新的MYOC Gly244Val变体的复合杂合子。

结论

虽然在白种人中发现了Gly252Arg的共同始祖，但这个携带MYOC突变的澳大利亚家系的表型比先前描述的要轻。由Gly252Arg突变引起的青光眼严重程度可能与Thr377Met MYOC突变相似，但比最常见的Gln368Stop突变更严重。

临床意义

自从其与青光眼相关联以来，已经开展了许多工作来研究与MYOC相关的青光眼的临床特征。鉴于与MYOC致病变体有很强的基因型 - 表型相关性，掌握此类分子信息的医疗保健专业人员能够准确地向患者提供有关其可能的病程的咨询。我们的研究表明，与MYOC Gly252Arg相关的疾病比先前在其他携带此特定突变的家系中描述的要轻。