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在青少年开角型青光眼中检测到一种新生的MYOC突变,该突变与房水中肌纤蛋白减少有关。

A de novo MYOC mutation detected in juvenile open angle glaucoma associated with reduced myocilin protein in aqueous humor.

作者信息

Kuchtey John, Chowdhury Uttio Roy, Uptegraft Colby C, Fautsch Michael P, Kuchtey Rachel W

机构信息

Vanderbilt Eye Institute, Vanderbilt University, 2311 Pierce Avenue, Nashville, TN 37232, USA.

出版信息

Eur J Med Genet. 2013 Jun;56(6):292-6. doi: 10.1016/j.ejmg.2013.03.002. Epub 2013 Mar 19.

Abstract

MYOC mutations were originally identified in patients with juvenile open angle glaucoma (JOAG). Cell culture and mouse studies suggest that MYOC mutations cause glaucoma through a dominant-negative effect on myocilin protein secretion. We tested this hypothesis with patient samples in this study. Glaucoma and control patients underwent complete ocular examination. DNA samples from glaucoma patients, unaffected relatives and controls were used for DNA sequencing of MYOC. Aqueous humor (AH) samples from glaucoma and control patients were obtained at the time of surgery. Myocilin protein in AH was detected by quantitative Western blot analysis. A de novo Val251Ala mutation of MYOC was found to segregate with disease in a family with autosomal dominant JOAG. Myocilin protein was detected in all control AH samples but was nearly undetectable in AH samples from a patient heterozygous for the Val251Ala mutation. Our results using human patient samples are consistent with a dominant-negative effect of pathogenic MYOC mutations on myocilin secretion.

摘要

MYOC突变最初是在青少年开角型青光眼(JOAG)患者中发现的。细胞培养和小鼠研究表明,MYOC突变通过对肌纤蛋白分泌的显性负效应导致青光眼。在本研究中,我们用患者样本检验了这一假设。青光眼患者和对照患者均接受了全面的眼部检查。来自青光眼患者、未受影响的亲属和对照的DNA样本用于MYOC的DNA测序。在手术时获取青光眼患者和对照患者的房水(AH)样本。通过定量蛋白质免疫印迹分析检测AH中的肌纤蛋白。在一个常染色体显性JOAG家族中,发现MYOC的一个新生Val251Ala突变与疾病相关。在所有对照AH样本中均检测到肌纤蛋白,但在Val251Ala突变杂合的患者的AH样本中几乎检测不到。我们使用人类患者样本的结果与致病性MYOC突变对肌纤蛋白分泌的显性负效应一致。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1233/3672363/4cd4925b7497/nihms459614f1.jpg

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