Introduction

Molecular Medicine Reports

1791-2997 1791-3004

D.A. Spandidos

10.3892/mmr.2016.5557

mmr-14-03-2439

Articles

Molecular analysis of myocilin and optineurin genes in Korean primary glaucoma patients

Park

Joonhong

12 Kim

Myungshin

12 Park

Chan Kee

3 Chae

Hyojin

12 Lee

Seungok

12 Kim

Yonggoo

12 Jang

Woori

12 Chi

Hyun Young

4 Park

Hae-Young Lopilly

3 Park

Shin Hae

1Department of Laboratory Medicine 2Catholic Genetic Laboratory Center, Seoul St. Mary's Hospital 3Department of Ophthalmology and Visual Science, College of Medicine, The Catholic University of Korea, Seoul 06591 4Department of Laboratory Medicine, Samkwang Medical Laboratories, Seoul 06742, Republic of Korea

Correspondence to: Dr Myungshin Kim, Department of Laboratory Medicine, College of Medicine, The Catholic University of Korea, 222 Banpo-daero, Seocho-gu, Seoul 06591, Republic of Korea, E-mail: microkim@catholic.ac.kr Dr Chan Kee Park, Department of Ophthalmology and Visual Science, College of Medicine, The Catholic University of Korea, 222 Banpo-daero, Seocho-gu, Seoul 06591, Republic of Korea, E-mail: ckpark@catholic.ac.kr

09 2016

27 07 2016

14 3 2439 2448 20 09 2015 27 06 2016

2016

This is an open access article distributed under the terms of the Creative Commons Attribution-NonCommercial-NoDerivs License, which permits use and distribution in any medium, provided the original work is properly cited, the use is non-commercial and no modifications or adaptations are made.

To investigate the underlying genetic influences of primary glaucoma in Korea, molecular analysis was performed in 112 sporadic cases, and results compared with healthy controls. The myocilin (MYOC) and optineurin (OPTN) genes were directly sequenced in 112 unrelated patients, including 17 with primary open-angle glaucoma, 19 with juvenile open-angle glaucoma, and 76 with normal tension glaucoma. Healthy unrelated Korean individuals (n=100) were used as the non-selected population control. A total of three MYOC and four OPTN variants potentially associated with primary glaucoma were identified in 4 and 18 patients, respectively. A novel variant of MYOC, p.Leu255Pro, was predicted to be potentially pathogenic by in silico analysis. Another, p.Thr353Ile, has been previously reported. These two missense variants were detected in patients with a family history of glaucoma. Combined heterozygous variants p.[Thr123=;Ile288=] were identified in 2 of 112 (2%) patients but not in healthy controls. Among OPTN variants, a novel variant p.Arg271Cys was identified. Homozygous p.[Thr34=;Thr34=] (4/112, 4%), homozygous p.[Met98Lys;Met98Lys] (4/112, 4%), or combined heterozygous p.[Thr34=;Arg545Gln] (9/112, 8%) was significantly associated with the development of primary glaucoma [odds ratio (OR)=8.768, 95% confidence interval (CI)=1.972–38.988; relative risk=1.818, 95% CI=1.473–2.244; P=0.001]. The present study provides insight into the genetic or haplotype variants of MYOC and OPTN genes contributing to primary glaucoma. Haplotype variants identified in the present study may be regarded as potential contributing factors of primary glaucoma in Korea. Further studies, including those on additional genes, are required to elucidate the underlying pathogenic mechanism using a larger cohort to provide additional statistical power.

primary glaucoma molecular analysis myocilin optineurin mutation

Introduction

Glaucoma is a complex, heterogeneous ocular disorder with multifactorial etiology characterized by structural damage to the optic nerve, visual field defects (1) and commonly relatively high intraocular pressure (IOP) (2). It is a leading cause of irreversible blindness worldwide (3,4) with ~20% of cases occurring secondary to other ocular or systemic diseases (1). Based on anatomical changes in the anterior chamber angle, primary glaucoma may be classified as primary angle closure glaucoma (PACG) or primary open-angle glaucoma (POAG), which may be further subdivided into juvenile open-angle glaucoma (JOAG) and adult onset POAG (1,5). Glaucoma is a treatable disease if detected early; however, many patients are diagnosed during routine examinations or only following advanced field loss, as glaucoma is typically asymptomatic in the early stages. Therefore, the development of an accurate test for the detection of presymptomatic carriers at risk is important for the management of glaucoma.

A family history of glaucoma is a well-known risk factor. Therefore genetic background is considered important for the development of the disease (6–8). The following genes have been reported to be associated with primary glaucoma: myocilin (MYOC) (9), optineurin (OPTN) (10), WD repeat domain 36 (11,12), neurotrophin 4 (13), optic atrophy 1 (14,15), cytochrome P450 family 1 subfamily B member 1 (16) and latent transforming growth factor β (17). To date, mutations in these genes account for only ~5% of patients with POAG (18), and the influence of mutations in these genes on patients with PACG remain controversial (19). The MYOC gene, located at the GLC1A locus on chromosome 1q24.3–q25.2, has been confirmed to be associated with JOAG and POAG, although mutation frequencies vary between ethnic groups (20). The altered protein product secreted into the extracellular matrix of the trabecular meshwork causes a severe form of autosomal dominant JOAG associated with very high IOP (9). Although up to 20% of JOAG may be associated with MYOC mutations, mutations in this gene have been identified in only 3 to 5% of POAG patients (7,21). Mutations in the OPTN gene, located at the GLC1E locus on chromosome 10p14–p15, result in normal tension glaucoma (NTG) without elevated IOP, a subtype of POAG (10).

To investigate the underlying genetic influences of primary glaucoma, molecular analysis of the MYOC and OPTN genes was performed in 112 Korean sporadic primary glaucoma patients, with the results compared to healthy controls.

Patients and methods Patients

All 112 patients with primary glaucoma from unrelated Korean patients were recruited from the ophthalmology clinic of Seoul St. Mary's Hospital (Seoul, Korea), including 17 POAG, 19 JOAG and 76 NTG patients. Healthy, unrelated Korean individuals (n=100) served as the non-selected population control. All patients and healthy controls in the study provided written informed consent for clinical and molecular analyses, and the study protocol was approved by the institutional review board of The Catholic University of Korea (Seoul, Korea). The diagnostic criteria of POAG were an IOP >21 mmHg by Goldmann applanation tonometry (GAT), presence of glaucomatous visual field defect or glaucomatous optic neuropathy and open angle. Where onset occurred at 5–35 years of age, patients were diagnosed with JOAG (22). The diagnostic criteria of NTG were an IOP <22 mmHg by GAT, presence of glaucomatous visual field defect or glaucomatous optic neuropathy and open angle. Patients with secondary glaucoma resulting from trauma, uveitis, neovascular or steroid-induced glaucoma (SIG), and other associated ocular or systemic anomalies were excluded from the present study. Healthy controls had IOP <20 mmHg, a normal optic disc appearance without suspicious glaucomatous changes, and no family or personal history of primary glaucoma.

Molecular analysis of the MYOC and OPTN genes

Genomic DNA samples were extracted from the peripheral blood using the QIAamp DNA Mini kit (Qiagen GmbH, Hilden, Germany). Entire coding exons and flanking intronic sequences of MYOC and OPTN were amplified by polymerase chain reaction (PCR) using different combinations of forward and reverse primers designed by the authors (Table I). Briefly, the PCR reaction had a total volume of 15 μl, comprising 10 μl Taq PCR Master Mix kit (Qiagen GmbH) containing Taq DNA Polymerase, 2X Qiagen PCR Buffer, 3 mM MgCl₂, and 400 μM of each deoxynucleotide, 2 μl 5X Q-Solution, 1 μl primer mix, and 2 μl genomic DNA (50 ng/μl). The PCR was amplified with a C1000 thermal cycler (Bio-Rad Laboratories, Inc., Hercules, CA, USA) under the following conditions: 5 min at 95°C, followed by 35 cycles of 95°C for 30 sec, 60°C for 30 sec and 72°C for 1 min, and a final step of 72°C for 5 min. Direct sequencing of PCR products was performed with the BigDye Terminator version 3.1 Cycle Sequencing kit (Applied Biosystems; Thermo Fisher Scientific, Inc., Waltham, MA, USA) and the products were resolved on ABI 3130XL Genetic Analyzer (Applied Biosystems; Thermo Fisher Scientific, Inc.). The resulting sequence electropherogram was analyzed using Sequencher software version 4.9 (Gene Codes Corporation, Ann Arbor, MI, USA). Sequence data were analyzed using reference sequences in GenBank (www.ncbi.nlm.nih.gov/genbank/). The RefSeq IDs NM_000261.1 for MYOC and NM_001008211.1 for OPTN were used for cDNA nucleotide numbering. All identified variants were confirmed by bidirectional resequencing.

Genetic variations were contrasted with Human Gene Mutation Database Public (www.hgmd.cf.ac.uk), 1,000 genomes project browser (browser.1000genomes.org) and the single nucleotide polymorphism database (www.ncbi.nlm.nih.gov/projects/SNP). Mutation pathogenicity was predicted through PolyPhen-2 version 2.2.2 (genetics.bwh.harvard.edu/pph2) (23) and PROVEAN version 1.1 (provean.jcvi.org) (24), the first predictor that includes in-frame insertions/deletions. To assess the extent of conservation of a novel variant of MYOC and OPTN hypothesized to be associated with disease, the amino acid sequence was aligned with protein sequences of various mammalian species using Clustal Omega software (www.ebi.ac.uk/Tools/msa/clustalo/) (25).

Haplotype analysis of the MYOC and OPTN genes

Haplotypes of each gene were constructed based on the genotype data of the MYOC and OPTN variants obtained from the 112 patients and 100 healthy controls. Haplotype reconstruction and frequency estimation were performed using haplo.em, an implementation of an Expectation-Maximization algorithm included in the R package haplo.stats, which computes maximum likelihood estimates of haplotype probabilities from unphased genotypes measured on unrelated individuals (R Foundation for Statistical Computing, Vienna, Austria; www.r-project.org). The frequencies of variant status between the patients and healthy controls were compared by χ² or Fisher's exact test using MedCalc software version 12.7.2 (MedCalc Software bvba, Ostend, Belgium). P<0.05 was considered to indicate a statistically significant difference.

Results

A total of three MYOC and four OPTN variants potentially associated with primary glaucoma were identified in 4 and 18 patients, respectively (Table II).

Molecular analysis of MYOC

Missense variants of MYOC were identified in two JOAG patients (P107 and P044) with a family history of primary glaucoma (pedigree analysis of P107 is presented in Fig. 1A). One was determined to be a novel missense variant, p.Leu255Pro, (P107; Fig. 1B) which was predicted to be 'probably damaging' with a score of 0.970 by PolyPhen-2 and was expected to be 'deleterious' with a score of −2.887 by PROVEAN. The position of changed amino acid was conserved among other mammalian species (Fig. 1C). No healthy control exhibited the same variant. The other variant identified, p.Thr353Ile, has previously been reported in Korean POAG (26). In addition, combined heterozygous variants p.[Thr123=;Ile288=] were identified in 2 of 112 (2%) patients but not in healthy controls; p.Thr123=[rs75682756; minor allele frequency (MAF)/minor allele count (MAC) by 1000 Genomes=0.0014/7], p.Ile288=(rs181923440; MAF/MAC=0.0010/5). The MYOC promoter variant c.-83G>A (rs2075648; MAF/MAC=0.1380/691) was detected only as a heterozygous state in a JOAG patient with p.Leu255Pro and in five NTG patients, but not in the 100 healthy controls (Table III). Clinical manifestations of primary glaucoma with MYOC are summarized in Table IV.

Molecular analysis of OPTN

OPTN variants were identified in 18 patients with primary glaucoma. One patient (P086) harbored a novel variant, p.Arg271Cys as a heterozygous state (Fig. 2A). This variant was predicted to be 'benign' with a score of 0.047 by PolyPhen-2 and was expected to be 'neutral' with a score of −1.726 by PROVEAN. This protein sequence was not highly conserved across the compared species, and the sequence in chicken had a cysteine in that position (Fig. 2B). One novel synonymous variant, p.Leu568=; c.1704A>G was identified in heterozygosity. These two variants were not detected in healthy controls.

In addition, three reported variants associated with primary glaucoma (10,27), including p.Thr34=(rs2234968), p.Met98Lys (rs11258194) and p.Arg545Gln (rs75654767) were identified (Table V). The p.Thr34=, p.Met98Lys and p.Arg545Gln mutations were detected in 40 (36%), 19 (17%), and 10 (9%) patients with primary glaucoma as well as in 25 (25%), 18 (18%), and 2 (2%) healthy controls, respectively, in a heterozygous or homozygous state. The odds ratio (OR) was not statistically different for p.Thr34= and p.Met98Lys by the χ² test (P=0.061 and P=0.492, respectively); however, it was significant for p.Arg545Gln by Fisher's exact test [OR=4.804, 95% confidence interval (CI)=1.026–22.482; relative risk=1.634, 95% CI=1.226–2.178; P=0.037]. The presence of one of homozygous p.[Thr34=;Thr34=] (4/112; 4%), homozygous p.[Met98Lys;Met98Lys] (4/112; 4%) or combined heterozygous p.[Thr34=;Arg545Gln] (9/112, 8%) was significantly associated with the development of primary glaucoma (OR=8.768, 95% CI=1.972–38.988; relative risk=1.818, 95% CI=1.473–2.244; P=0.001). Clinical manifestations of primary glaucoma with OPTN variants are summarized in Table VI.

Discussion

The present study reports a molecular analysis of MYOC and OPTN genes in 112 patients with primary glaucoma. One novel MYOC variant, p.Leu255Pro, in patient P107 with a family history of glaucoma was predicted to have a deleterious effect by in silico analysis. This variant is a possible pathogenic mutation associated with the development of primary glaucoma. The second MYOC variant, p.Thr353Ile, in patient P044 with a family history of glaucoma has been previously reported as a pathologic mutation for POAG and resides in the olfactomedin-homology region. It may be involved in the regulation of IOP in trabecular-meshwork cells (26). The presence of heterozygous p.Thr123= and p.Ile288= was observed only in patients with JOAG and NTG. Thus, p.[Thr123=;Ile288=] may be a part of the haplotype variant associated with the development of primary glaucoma. Further extended haplotype analysis is required to confirm the association of MYOC haplotype variants. The variant in the 5′-UTR region, c.-83G>A, which was initially reported in Western countries (20,28), and subsequently observed in Hong Kong (29) and the Philippines (30), was identified only in primary glaucoma patients in the present study. The association of c.-83G>A and the risk of primary glaucoma remains controversial due to the variable frequency and the non-significant differences between POAG patients and controls observed in previous studies (28,31,32).

Genetic analysis of the OPTN coding region was performed in all patients with primary glaucoma. Notably, OPTN variants (10/76, 13.2%) were identified more frequently than MYOC variants (1/76, 1.3%) in NTG patients, which is consistent with previous studies (33,34). The three OPTN variants p.Thr34=, p.Leu40= and p.Glu89His were identified in 7 of 53 Korean NTG patients (33), whereas only one patient with the MYOC variant p.Leu411= was reported from 32 separate Korean NTG patients (34). Supporting the findings of the present study, Rezaie et al (10) suggested that mutations in OPTN may be responsible for 16.7% of the hereditary forms of NTG and that there is an additional risk factor of 13.6% in familial and sporadic cases. Furthermore, Sohn et al (35) demonstrated that the MYOC gene itself was not associated with OAG, including POAG, NTG and SIG. Their results do not support the hypothesis that MYOC induction may be linked to IOP variation and that promoter variants of MYOC may be a risk factor for the pathogenesis of OAG.

A novel OPTN variant, p.Arg271Cys, of unknown significance was identified in patient P086 with NTG (1/112, 1%). This variant led to replacement of arginine with cysteine at codon 271, however, the protein sequence was not highly conserved across species. Although this variant was predicted to be 'benign' or 'neutral', it is potentially pathogenic as it was not present in the healthy controls. Segregation analysis and/or functional studies are required to verify the pathogenicity or neutrality of this variant.

Of the OPTN haplotype variants, p.Thr34=, p.Met98Lys and p.Arg545Gln have been previously reported as possible glaucoma-causing mutations (10,27). However, they were present at reduced frequencies as a heterozygous state in healthy controls.

The p.Thr34= variant was detected in 40 of 112 (36%) patients with primary glaucoma and in 25 of 100 (25%) healthy controls in a heterozygous or homozygous state in the present study. Homozygosity for p.Thr34= was observed only in four patients with primary glaucoma (P059, P060, P098 and P109). Funayama et al (27) reported that p.Thr34= was weakly associated with patients with OAG with elevated IOP, whereas p.Met98Lys was weakly associated with patients with OAG with normal IOP. In interaction analysis between olfactomedin 2 (OLFM2) and OPTN genes in patients with OAG, the c.317G>A; p.Arg106Gln of OLFM2 and c.412G>A; p.Thr34= of OPTN and the c.1281C>T; p.Arg427Arg of OLFM2 and c.412G>A; p.Thr34= of OPTN were significantly associated with OAG with elevated IOP. These results suggest that these variants in OLFM2 and OPTN contribute interactively to OAG, indicating a polygenic etiology with different properties for p.Thr34= and p.Met98Lys variants of OPTN.

The p.Met98Lys variant was identified in 19 of 112 (17%) patients with primary glaucoma as well as in 18 of 100 (18%) healthy controls as a heterozygous or homozygous state in the present study. Alward et al (36) and Fuse et al (37) reported a significant association between p.Met98Lys and glaucoma in Japanese patients. By contrast, Toda et al (38) identified similar frequencies of p.Met98Lys in Japanese glaucoma patients and controls. Notably, p.Met98Lys has been demonstrated to be a polymorphic variant in German, French and Moroccan patients (39,40). By contrast to previous studies (10,41,42), the frequency difference in the present study (4 vs. 0%) between the patients with homozygous p.Met98Lys (P014, P029, P054 and P058) and healthy controls was highly significant. p.Met98Lys is located within a putative basic leucine zipper domain and is conserved in macaques; it may represent a risk associated factor or a dominant susceptibility allele (10). Wild-type OPTN protein, operating through the tumor necrosis factor α pathway, may have a neuroprotective role in the eye and optic nerve; however when defective, it produces visual loss and optic neuropathy as typically observed in normal and high-pressure glaucoma (10).

The p.Arg545Gln variant was reported previously in POAG families with normal IOP (10). Although the p.Arg545Gln variant is not part of a known protein domain, it is situated near the only zinc finger motif within OPTN. This motif is typically observed in transcription factors. p.Arg545Gln has been detected in similar frequencies in Japanese glaucoma patients and healthy controls (38). Alward et al (36) suggested that p.Arg545Gln may not be a disease-causing polymorphism. Results concerning the effect of OPTN on glaucoma have been equivocal (10,32,43,44); however, the expression of MYOC may be regulated by OPTN (45). Notably, results from the present study support the view that the three variants of OPTN may be involved in the development of primary glaucoma, as the OR for the haplotype harboring homozygous p.Thr34= or p.Met98Lys as well as a simultaneous presence of heterozygous p.Thr34= and p.Arg545Gln was statistically significant by the Fisher's exact test (OR=8.768, 95%, CI=1.972–38.988; relative risk=1.818, 95% CI=1.473–2.244; P=0.001).

In conclusion, haplotype variants identified in the present study may be regarded as potential contributing factors for primary glaucoma in Korea. The present study provides insight into the genetic or haplotype variants contributing to primary glaucoma. Further studies, including on additional genes, are required to elucidate the underlying pathogenic mechanism using larger cohorts to provide additional statistical power.

Acknowledgments

The authors would like to thank The Catholic Genetic Laboratory Center (Seoul, Korea) for its assistance in conducting the present study and compiling this report. The present study was supported by a grant from the Basic Science Research Program through the National Research Foundation of Korea (Daejeon, Korea; grant no. NRF-2013R1A1A2006801) funded by the Ministry of Education (Sejong, Korea).

References 1

Foster

Buhrmann

Quigley

Johnson

The definition and classification of glaucoma in prevalence surveys

Br J Ophthalmol862382422002

10.1136/bjo.86.2.238

11815354

1771026

Pakravan

Yazdani

Javadi

Amini

Behroozi

Ziaei

Katibeh

Solaimanizad

Ghahari

Yaseri

A population-based survey of the prevalence and types of glaucoma in central Iran: The Yazd eye study

Ophthalmology120197719842013

10.1016/j.ophtha.2013.02.029

23664464

Casson

Chidlow

Wood

Crowston

Goldberg

Definition of glaucoma: Clinical and experimental concepts

Clin Experiment Ophthalmol403413492012

10.1111/j.1442-9071.2012.02773.x

22356435

Weinreb

Aung

Medeiros

The pathophysiology and treatment of glaucoma: A review

JAMA311190119112014

10.1001/jama.2014.3192

24825645

4523637

Goldwyn

Waltman

Becker

Primary open-angle glaucoma in adolescents and young adults

Arch Ophthalmol845795821970

10.1001/archopht.1970.00990040581004

5478882

Booth

Churchill

Anwar

Menage

Markham

The genetics of primary open angle glaucoma

Br J Ophthalmol814094141997

10.1136/bjo.81.5.409

9227209

1722199

Wiggs

Genetic etiologies of glaucoma

Arch Ophthalmol12530372007

10.1001/archopht.125.1.30

17210849

Khan

Genetics of primary glaucoma

Curr Opin Ophthalmol223473552011

10.1097/ICU.0b013e32834922d2

21730848

Stone

Fingert

Alward

Nguyen

Polansky

Sunden

Nishimura

Clark

Nystuen

Nichols

Identification of a gene that causes primary open angle glaucoma

Science2756686701997

10.1126/science.275.5300.668

9005853

Rezaie

Child

Hitchings

Brice

Miller

Coca-Prados

Héon

Krupin

Ritch

Kreutzer

Adult onset primary open-angle glaucoma caused by mutations in optineurin

Science295107710792002

10.1126/science.1066901

11834836

Monemi

Spaeth

DaSilva

Popinchalk

Ilitchev

Liebmann

Ritch

Héon

Crick

Child

Sarfarazi

Identification of a novel adult-onset primary open-angle glaucoma (POAG) gene on 5q22.1

Hum Mol Genet147257332005

10.1093/hmg/ddi068

15677485

Footz

Johnson

Dubois

Boivin

Raymond

Walter

Glaucoma-associated WDR36 variants encode functional defects in a yeast model system

Hum Mol Genet18127612872009

10.1093/hmg/ddp027

19150991

Pasutto

Matsumoto

Mardin

Sticht

Brandstätter

Michels-Rautenstrauss

Weisschuh

Gramer

Ramdas

van Koolwijk

Heterozygous NTF4 mutations impairing neurotrophin-4 signaling in patients with primary open-angle glaucoma

Am J Hum Genet854474562009

10.1016/j.ajhg.2009.08.016

19765683

2756554

Aung

Ocaka

Ebenezer

Morris

Krawczak

Thiselton

Alexander

Votruba

Brice

Child

A major marker for normal tension glaucoma: Association with polymorphisms in the OPA1 gene

Hum Genet11052562002

10.1007/s00439-001-0645-7

11810296

Guo

Chen

Zhang

Yang

Cheng

Zhao

Association of OPA1 polymorphisms with NTG and HTG: A meta-analysis

PLoS One7e423872012

10.1371/journal.pone.0042387

22879959

3411762

Kaur

Mandal

Chakrabarti

Primary congenital glaucoma and the involvement of CYP1B1

Middle East Afr J Ophthalmol187162011

10.4103/0974-9233.75878

21572728

3085158

Jelodari-Mamaghani

Haji-Seyed-Javadi

Suri

Nilforushan

Yazdani

Kamyab

Elahi

Contribution of the latent transforming growth factor-β binding protein 2 gene to etiology of primary open angle glaucoma and pseudoexfoliation syndrome

Mol Vis193333472013

3568400

Fingert

Primary open-angle glaucoma genes

Eye (Lond)255875952011

10.1038/eye.2011.97

Shastry

Genetic susceptibility to primary angle closure glaucoma (PACG)

Discov Med1517222013

23375010

Fingert

Héon

Liebmann

Yamamoto

Craig

Rait

Kawase

Hoh

Buys

Dickinson

Analysis of myocilin mutations in 1703 glaucoma patients from five different populations

Hum Mol Genet88999051999

10.1093/hmg/8.5.899

10196380

Menaa

Braghini

Vasconcellos

Menaa

Costa

Figueiredo

Melo

Keeping an eye on myocilin: A complex molecule associated with primary open-angle glaucoma susceptibility

Molecules16540254212011

10.3390/molecules16075402

21709622

Turalba

Chen

Clinical and genetic characteristics of primary juvenile-onset open-angle glaucoma (JOAG)

Semin Ophthalmol2319252008

10.1080/08820530701745199

18214788

Adzhubei

Schmidt

Peshkin

Ramensky

Gerasimova

Bork

Kondrashov

Sunyaev

A method and server for predicting damaging missense mutations

Nat Methods72482492010

10.1038/nmeth0410-248

20354512

2855889

Choi

Sims

Murphy

Miller

Chan

Predicting the functional effect of amino acid substitutions and indels

PLoS One7e466882012

10.1371/journal.pone.0046688

23056405

3466303

Sievers

Wilm

Dineen

Gibson

Karplus

Lopez

McWilliam

Remmert

Söding

Fast, scalable generation of high-quality protein multiple sequence alignments using Clustal Omega

Mol Syst Biol75392011

10.1038/msb.2011.75

21988835

3261699

Yoon

Kim

Moon

Lim

Joo

Mutations of the TIGR/MYOC gene in primary open-angle glaucoma in Korea

Am J Hum Genet64177517781999

10.1086/302407

10330365

1377921

Funayama

Mashima

Ohtake

Ishikawa

Fuse

Yasuda

Fukuchi

Murakami

Hotta

Shimada

Glaucoma Gene Research Group

SNPs and interaction analyses of noelin 2, myocilin, and optineurin genes in Japanese patients with open-angle glaucoma

Invest Ophthalmol Vis Sci47536853752006

10.1167/iovs.06-0196

17122126

Alward

Fingert

Coote

Johnson

Lerner

Junqua

Durcan

McCartney

Mackey

Sheffield

Stone

Clinical features associated with mutations in the chromosome 1 open-angle glaucoma gene (GLC1A)

N Engl J Med338102210271998

10.1056/NEJM199804093381503

9535666

Fan

Leung

Pang

Baum

Tam

Wang

Lam

Single nucleotide polymorphisms of the myocilin gene in primary open-angle glaucoma patients

Zhonghua Yi Xue Yi Chuan Xue Za Zhi2170732004

14767915

Wang

Fan

Canlas

Tam

Ritch

Lam

Fan

Pang

Absence of myocilin and optineurin mutations in a large Philippine family with juvenile onset primary open angle glaucoma

Mol Vis108518562004

15547491

Mukhopadhyay

Acharya

Mukherjee

Ray

Choudhury

Khan

Ray

Mutations in MYOC gene of Indian primary open angle glaucoma patients

Mol Vis84424482002

12447164

Kumar

Basavaraj

Gupta

Qamar

Ali

Bajaj

Ramesh

Prakash

Shetty

Dorairaj

Role of CYP1B1, MYOC, OPTN, and OPTC genes in adult-onset primary open-angle glaucoma: Predominance of CYP1B1 mutations in Indian patients

Mol Vis136676762007

17563717

2765475

Jeong

Kim

Mun

Kee

OPTN gene mutation in normal-tension glaucoma

J Korean Ophthalmol Soc44190319072003

Lee

Hur

Kee

Analysis of TIGR gene mutation in glaucoma

J Korean Ophthalmol Soc41109511012000

Sohn

Hur

Choi

Chung

Kee

Little evidence for association of the glaucoma gene MYOC with open-angle glaucoma

Br J Ophthalmol946396422010

10.1136/bjo.2009.158261

20447966

2976471

Alward

Kwon

Kawase

Craig

Hayreh

Johnson

Khanna

Yamamoto

Mackey

Roos

Evaluation of optineurin sequence variations in 1,048 patients with open-angle glaucoma

Am J Ophthalmol1369049102003

10.1016/S0002-9394(03)00577-4

14597044

Fuse

Takahashi

Akiyama

Nakazawa

Seimiya

Kuwahara

Tamai

Molecular genetic analysis of optineurin gene for primary open-angle and normal tension glaucoma in the Japanese population

J Glaucoma132993032004

10.1097/00061198-200408000-00007

15226658

Toda

Tang

Kashiwagi

Mabuchi

Iijima

Tsukahara

Yamagata

Mutations in the optineurin gene in Japanese patients with primary open-angle glaucoma and normal tension glaucoma

Am J Med Genet A125A142004

10.1002/ajmg.a.20439

14755458

Melki

Belmouden

Akhayat

Brézin

Garchon

The M98K variant of the OPTINEURIN (OPTN) gene modifies initial intraocular pressure in patients with primary open angle glaucoma

J Med Genet408428442003

10.1136/jmg.40.11.842

14627677

1735315

Weisschuh

Neumann

Wolf

Wissinger

Gramer

Prevalence of myocilin and optineurin sequence variants in German normal tension glaucoma patients

Mol Vis112842872005

15851979

Mukhopadhyay

Komatireddy

Acharya

Bhattacharjee

Mandal

Thakur

Chandrasekhar

Banerjee

Thomas

Chakrabarti

Ray

Evaluation of Optineurin as a candidate gene in Indian patients with primary open angle glaucoma

Mol Vis117927972005

16205626

Sripriya

Nirmaladevi

George

Hemamalini

Baskaran

Prema

Ve Ramesh

Karthiyayini

Amali

Job

OPTN gene: Profile of patients with glaucoma from India

Mol Vis128168202006

16885925

Tektas

Lütjen-Drecoll

Structural changes of the trabecular meshwork in different kinds of glaucoma

Exp Eye Res887697752009

10.1016/j.exer.2008.11.025

Cheng

Cai

Wei

The prevalence of primary glaucoma in mainland China: A systematic review and meta-analysis

J Glaucoma223013062013

10.1097/IJG.0b013e31824083ca

Huang

Guo

Xiao

Jia

Liu

Zhang

Mutation analysis of seven known glaucoma-associated genes in Chinese patients with glaucoma

Invest Ophthalmol Vis Sci55359436022014

10.1167/iovs.14-13927

24825108

Figure 1

(A)Pedigree analysis of patient P107 diagnosed with juvenile open-angle glaucoma, with a novel missense variant p.Leu255Pro. Proband (indicated by the arrow) and affected family members revealed the same mutation in the heterozygous state. (B) Partial sequence of exon3 of MYOC revealed a heterozygous single-base substitution (c.764T>C) leading to missense variant p.Leu255Pro in patient P107. (C) Alignment of MYOC amino acid sequences in human and other species. The position of the changed amino acid in the patient with glaucoma identified in the present study is underlined. The conservation of p.Leu255Pro was assumed by protein alignment of various MYOC orthologs using Clustal Omega software. MYOC, myocilin.

Figure 2

(A) Partial sequence of exon9 of OPTN revealed a heterozygous single-base substitution (c.811C>T) leading to missense variant p.Arg271Cys in patient P086 with normal tension glaucoma. (B) Alignment of OPTN amino acid sequences in human and other mammalian species. The position of the changed amino acid in the patient with glaucoma identified in the present study is underlined. The conservation of p.Arg271Cys was assessed by protein alignment of various OPTN orthologs using Clustal Omega. OPTN, optineurin.

Table I

Oligonucleotide primer sequences used for mutation analysis of MYOC and OPTN genes.

Gene	Exon	Primer sequence (5′ to 3′)		Size (bp)
Gene	Exon	Forward	Reverse	Size (bp)
MYOC	1a	TCTTGCTGGCAGCGTG	CTGGTCCAAGGTCAATTGGT	626
MYOC	1b	AGCACCCAACGCTTAGACCT	TCTGTCTTGTGCTAGCTGTGC	497
MYOC	2	TGCCACCACATCCAGCTAAT	CTCTGCTCCCAGGGAAGTTA	495
MYOC	3a	ACCCAGACGATTTGTCTCCA	GCCTCATCGGTGCTGTAAAT	586
MYOC	3b	CGCTGAGTCCAGAACTGTCA	CGCCCTCAGACTACAATTCC	685
OPTN	1	CGGACAGCGAGGGTGGGTA	GCGGGTACCGTTTTCAGG	445
OPTN	2	TCCACATGGATGCCTCTACA	TTCCCATGCAAATCTTCAAA	459
OPTN	3	TGTTAGCCAGGATGGTCTCA	AGAGGTTGATGGGACATTGC	391
OPTN	4	CACACACACACTTTTCTGAAGC	CCCCACCAGCTACCACCTAT	497
OPTN	5	CTTCGTCTTTTTGCTGCTGA	CTTCCAAGACCAGGCAAAAC	492
OPTN	6	TGTAAAGATGGGGGTCTTGC	GAAAATGAGAGCCAATTTATCTTTG	491
OPTN	7	CTTGGGTTGCATGTCACAAA	CAGTGTGAGCCAAACAGGAA	398
OPTN	8	GACCAGCTGTGCTTGTTCAC	CAGACAGTGAGTGCTGTTTGG	495
OPTN	9	TTTCACTTGCCTTTTACCTCTG	GACACAGAGCAGGACAAGGA	498
OPTN	10	TTGGGGTATTGTCAAAGTTGG	ATGCCCCTAAATGGCAGAAT	486
OPTN	11	TCATAAACCCTACAGCCCTAAAA	TGCTAGGACTCCTTCAGATAAGTG	398
OPTN	12	GCTAGTAGGTCGTGGGGTGA	GGAAAACAACCTTTGAAACCA	346
OPTN	13	CCGGCCAGAGCTGATAAT	TTTTAATACACTCACGGGTGAAA	394
OPTN	14	AGCAGGATTGTGCATCTGTG	GCGCGAACACAGCTATTCTT	369
OPTN	15	GGTTTTTATGAACCTTGGCAGT	GATTCGGTGGGTAATGGATG	381
OPTN	16	TGCATCGTGATGACTTCAGTT	CTCAAACCCTGACCCCAAGT	500

Table II

Frequencies of MYOC and OPTN variants identified in primary glaucoma.

Gene	Variant	Zygosity	Primary glaucoma, n=112			Healthy control, n=100
Gene	Variant	Zygosity	POAG, n=17	JOAG, n=19	NTG, n=76	Healthy control, n=100
MYOC	c.-83G>A and c.764T>C;p.Leu255Pro	Combined heterozygous	0	1	0	0
MYOC	c.1058C>T;p.Thr353Ile	Heterozygous	0	1	0	0
MYOC	c.369C>T;p.Thr123= and c.864C>T;p.Ile288=	Combined heterozygous	0	1	1	0
OPTN	c.102G>A; p.Thr34=	Homozygous	1	1	2	0
OPTN	c.293T>A;p.Met98Lys	Homozygous	1	1	2	0
OPTN	c.811C>T;p.Arg271Cys	Heterozygous	0	0	1	0
OPTN	c.102G>A;p.Thr34= and c.1634G>A;p.Arg545Gln	Combined heterozygous	2	2	5	2

JOAG, juvenile open-angle glaucoma; POAG, primary open-angle glaucoma; NTG, normal tension glaucoma; MYOC, myocilin; OPTN, optineurin.

Table III

Genotype frequencies of MYOC gene identified in korean patients with primary glaucoma.

Location	cDNA change	Protein change	Genotype frequencies (%)						rs IDs
Location	cDNA change	Protein change	Primary glaucoma, n=112			Normal control, n=100			rs IDs
5′-UTR	c.-83G>A	–	GG 106/112 (94.6)	GA 6/112 (5.4)	AA 0/112 (0)	GG 100/100 (100)	GA 0/100 (0)	AA 0/100 (0)	rs2075648
Exon1	c.57G>T	p.Gln19His	GG 110/112 (98.2)	GT 2/112 (1.8)	TT 0/112 (0)	GG 100/100 (100)	GT 0/100 (0)	TT 0/100 (0)	rs2234925
Exon1	c.227G>A	p.Arg76Lys	GG 102/112 (91.1)	GA 10/112 (8.9)	AA 0/112 (0)	GG 96/100 (96)	GA 4/100 (4)	AA 0/100 (0)	rs2234926
Exon1	c.369C>T	p.Thr123=	CC 110/112 (98.2)	CT 2/112 (1.8)	TT 0/112 (0)	CC 100/100 (100)	CT 0/100 (0)	TT 0/100 (0)	rs75682756
Exon2	c.624C>G	p.Asp208Glu	CC 109/112 (97.3)	CG 3/112 (2.7)	GG 0/112 (0)	CC 98/100 (98)	CG 2/100 (2)	GG 0/100 (0)	rs2234927
Exon3	c.764T>C	p.Leu255Pro	TT 111/112 (99.1)	TC 1/112 (0.9)	CC 0/112 (0)	TT 100/100 (100)	TC 0/100 (0)	CC 0/100 (0)	–
Exon3	c.864C>T	p.Ile288=	CC 110/112 (98.2)	CT 2/112 (1.8)	TT 0/112 (0)	CC 100/100 (100)	CT 0/100 (0)	TT 0/100 (0)	rs181923440
Exon3	c.1058C>T	p.Thr353Ile	CC 111/112 (99.1)	CT 1/112 (0.9)	TT 0/112 (0)	CC 100/100 (100)	CT 0/100 (0)	TT 0/100 (0)	rs137853277
Exon3	c.1464C>T	p.Ala488=	CC 111/112 (99.1)	CT 1/112 (0.9)	TT 0/112 (0)	CC 100/100 (100)	CT 0/100 (0)	TT 0/100 (0)	rs2234929
3′-UTR	c.^*73G>C	–	GG 103/112 (92)	GC 8/112 (7.1)	CC 1/112 (0.9)	GG 98/100 (98)	GC 1/100 (1)	CC 1/100 (1)	rs74403899

MYOC, myocilin; UTR, untranslated region; rs IDs, reference single nucleotide polymorphism identification numbers.

Table IV

Clinical manifestations in four primary glaucomas with MYOC variants.

Patient	Diagnosis	Variant 1	Variant 2	Sex	Age at Dx (year)	BCVA		Max IOP (mmHg)		VCDR		VFMD
Patient	Diagnosis	Variant 1	Variant 2	Sex	Age at Dx (year)	OD	OS	OD	OS	OD	OS	OD	OS
P107	JOAG	c.-83G>A	c.764T>C;p.Leu255Pro	F	14	1	0.04	39	40	0.6	0.8	−5.17	−5.32
P044	JOAG	c.1058C>T;p.Thr353Ile	None	F	12	1	0.8	27	26	0.6	0.6	−3.33	−4.24
P006	JOAG	c.369C>T;p.Thr123=	c.864C>T;p.Ile288=	M	28	1	1	23	23	0.5	0.6	−0.26	−1.11
P039	NTG	c.369C>T;p.Thr123=	c.864C>T;p.Ile288=	F	22	1	1	16	15	0.6	0.5	−1.07	−1.02

MYOC, myocilin; JOAG, juvenile open-angle glaucoma; NTG, normal tension glaucoma; M, male; F, female; Dx, diagnosis; BCVA, best corrected visual acuity; Max IOP, maximum intraocular pressure; VCDR, vertical cup-to-disc ratio; VFMD, visual field mean deviation; OD, oculus dexter; OS, oculus sinister.

Table V

Genotype frequencies of OPTN gene identified in Korean patients with primary glaucoma.

Location	cDNA change	Protein change	Genotype frequencies (%)						rs IDs
Location	cDNA change	Protein change	Primary glaucoma, n=112			Normal control, n=100			rs IDs
Exon4	c.102G>A	p.Thr34=	GG 72/112 (64.3)	GA 36/112 (32.1)	AA 4/112 (3.6)	GG 75/100 (75)	GA 25/100 (25)	AA 0/100 (0)	rs2234968
Exon4	c.147C>T	p.Thr49=	CC 111/112 (99.1)	CT 1/112 (0.9)	TT 0/112 (0)	CC 95/100 (95)	CT 5/100 (5)	TT 0/100 (0)	rs187734249
Exon5	c.293T>A	p.Met98Lys	TT 93/112 (83.1)	TA 15/112 (13.4)	AA 4/112 (3.5)	TT 82/100 (82)	TA 18/100 (18)	AA 0/100 (0)	rs11258194
Intron6	c.552+63C>T	–	CC 112/112 (100)	CT 0/112 (0)	TT 0/112 (0)	CC 99/100 (99)	CT 1/100 (1)	TT 0/100 (0)	rs184333348
Intron6	c.553-10G>A	–	GG 84/112 (75)	GA 20/112 (17.9)	AA 8/112 (7.1)	GG 66/100 (66)	GA 34/100 (34)	AA 0/100 (0)	rs11258210
Intron6	c.553-5C>T	–	CC 20/112 (17.9)	CT 39/112 (34.8)	TT 53/112 (47.3)	CC 7/100 (7)	CT 45/100 (45)	TT 48/100 (48)	rs2244380
Intron7	c.626+24G>A	–	GG 103/112 (92)	GA 7/112 (6.3)	AA 2/112 (1.8)	GG 90/100 (90)	GA 10/100 (10)	AA 0/100 (0)	rs11258211
Intron8	c.780-53T>C	–	TT 88/112 (78.6)	TC 22/112 (19.6)	CC 2/112 (1.8)	TT 89/100 (92)	TC 10/100 (10)	CC 1/100 (1)	rs765884
Exon9	c.811C>T	p.Arg271Cys	TT 111/112 (99.1)	CT 1/112 (0.9)	TT 0/112 (0)	TT 100/100 (100)	CT 0/100 (0)	TT 0/100 (0)	–
Intron9	c.882+19C>T	–	CC 111/112 (99.1)	CT 1/112 (0.9)	TT 0/112 (0)	CC 99/100 (99)	CT 1/100 (1)	TT 0/100 (0)	rs2277219
Exon10	c.964G>A	p.Glu322=	GG 111/112 (99.1)	GA 0/112 (0)	AA 1/112 (0.9)	GG 100/100 (100)	GA 0/100 (0)	AA 0/100 (0)	rs523747
Intron11	c.1149-86G>T	–	GG 28/112 (25)	GT 33/112 (29.5)	TT 51/112 (45.5)	GG 10/100 (10)	GT 41/100 (41)	TT 49/100 (49)	rs676302
Intron15	c.1613-48C>A	–	CC 64/112 (57.1)	CA 30/112 (26.8)	AA 18/112 (16.1)	CC 34/100 (34)	CA 50/100 (50)	AA 16/100 (16)	rs10906310
Exon16	c.1634G>A	p.Arg545Gln	GG 102/112 (91.1)	GA 10/112 (8.9)	AA 0/112 (0)	GG 98/100 (98)	GA 2/100 (2)	AA 0/100 (0)	rs75654767
Exon16	c.1704A>G	p.Leu568=	AA 111/112 (99.1)	AG 1/112 (0.9)	GG 0/112 (0)	AA 100/100 (100)	AG 0/100 (0)	GG 0/100 (0)	–

OPTN, optineurin; rs IDs, reference single nucleotide polymorphism identification numbers.

Table VI

Clinical manifestations in 18 primary glaucomas with OPTN variants.

Patient	Diagnosis	Variant 1	Variant 2	Sex	Age at Dx (year)	BCVA		Max IOP (mmHg)		VCDR		VFMD
Patient	Diagnosis	Variant 1	Variant 2	Sex	Age at Dx (year)	OD	OS	OD	OS	OD	OS	OD	OS
P059	JOAG	c.102G>A;p.Thr34=	c.102G>A;p.Thr34=	M	7	1	1	28	28	0.8	0.7	−1.52	−1.81
P060	POAG	c.102G>A;p.Thr34=	c.102G>A;p.Thr34=	F	47	0.1	0.1	25	25	0.6	0.6	−10.47	−12.93
P098	NTG	c.102G>A;p.Thr34=	c.102G>A;p.Thr34=	M	25	1	1	13	13	0.7	0.8	−4.08	−3.09
P109	NTG	c.102G>A;p.Thr34=	c.102G>A;p.Thr34=	M	34	1	1	16	17	0.7	0.6	−0.69	−1.38
P014	POAG	c.293T>A;p.Met98Lys	c.293T>A;p.Met98Lys	M	40	1	1	24	22	0.8	0.8	−12.88	−32.71
P029	JOAG	c.293T>A;p.Met98Lys	c.293T>A;p.Met98Lys	M	7	0.4	1	24	27	0.7	0.7	−8.32	−6.63
P054	NTG	c.293T>A;p.Met98Lys	c.293T>A;p.Met98Lys	M	29	0.8	0.8	19	19	0.6	0.4	−16.36	−2.2
P058	NTG	c.293T>A;p.Met98Lys	c.293T>A;p.Met98Lys	M	26	1	1	21	21	0.5	0.6	−0.04	−1.93
P086	NTG	c.811C>T;p.Arg271Cys	None	M	17	1	1	19	19	0.7	0.6	−1.46	−1.25
P003	POAG	c.102G>A;p.Thr34=	c.1634G>A;p.Arg545Gln	M	49	0.8	1	23	22	0.8	0.7	−3.42	−2.48
P010	NTG	c.102G>A;p.Thr34=	c.1634G>A;p.Arg545Gln	M	36	1	1	16	16	0.6	0.6	0.23	−0.95
P023	NTG	c.102G>A;p.Thr34=	c.1634G>A;p.Arg545Gln	F	28	0.8	1	17	18	0.7	0.5	−1.18	−3.25
P034	JOAG	c.102G>A;p.Thr34=	c.1634G>A;p.Arg545Gln	F	29	1	1	29	28	0.4	0.8	NA	NA
P049	NTG	c.102G>A;p.Thr34=	c.1634G>A;p.Arg545Gln	F	29	1	1	20	20	0.7	0.7	−3.75	−3.3
P066	NTG	c.102G>A;p.Thr34=	c.1634G>A;p.Arg545Gln	F	32	1	1	15	15	0.2	0.2	−4.66	−3.77
P081	JOAG	c.102G>A;p.Thr34=	c.1634G>A;p.Arg545Gln	M	15	1	1	23	22	0.5	0.5	−0.08	−0.54
P095	POAG	c.102G>A;p.Thr34=	c.1634G>A;p.Arg545Gln	M	43	1	1	31	31	0.6	0.7	−6.48	−4.35
P105	NTG	c.102G>A;p.Thr34=	c.1634G>A;p.Arg545Gln	F	43	1	1	21	21	0.6	0.6	−0.34	−0.18

OPTN, optineurin; JOAG, juvenile open-angle glaucoma; POAG, primary open-angle glaucoma; NTG, normal tension glaucoma; M, male; F, female; Dx, diagnosis; BCVA, best corrected visual acuity; Max IOP, maximum intraocular pressure; VCDR, vertical cup-to-disc ratio; VFMD, visual field mean deviation; OD, oculus dexter; OS, oculus sinister; NA, not available.