TY - JOUR
T1 - Genetic analysis of Japanese primary open-angle glaucoma patients and clinical characterization of risk alleles near CDKN2B-AS1, SIX6 and GAS7
AU - Japan Glaucoma Society Omics Group (JGS-OG)
AU - Shiga, Yukihiro
AU - Nishiguchi, Koji M.
AU - Kawai, Yosuke
AU - Kojima, Kaname
AU - Sato, Kota
AU - Fujita, Kosuke
AU - Takahashi, Mai
AU - Omodaka, Kazuko
AU - Araie, Makoto
AU - Kashiwagi, Kenji
AU - Aihara, Makoto
AU - Iwata, Takeshi
AU - Mabuchi, Fumihiko
AU - Takamoto, Mitsuko
AU - Ozaki, Mineo
AU - Kawase, Kazuhide
AU - Fuse, Nobuo
AU - Yamamoto, Masayuki
AU - Yasuda, Jun
AU - Nagasaki, Masao
AU - Nakazawa, Toru
N1 - Funding Information:
Funding: This paper was supported in part by the Japan Society For The Promotion Of Science KAKENHI Grants-in-Aid for Scientific Research (B) (T.N. 26293372) and by an unrestricted grant from Senju Pharmaceutical Co. Ltd., Osaka, Japan. Part of SNP genotyping was supported by the Center of Innovation Program from Japan Science and Technology Agency, JST. The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript. The authors thank Naoto Imadome, Hidetoshi Takahashi, Shota Ono, Ryosuke Wakusawa, Tomoki Yasui, Keiichi Kato, Hitoshi Okabe, Makoto Ohmura, Nobuo Maekawa, Yuya Sato, members of Japan Glaucoma Society Omics Group (Makoto Araie, Kenji Kashiwagi, Makoto Aihara, Takeshi Iwata, Fumihiko Mabuchi, Mistuko Takamoto, Mineo ozaki and Kazuhide Kawase) for their contribution in sample collection and Sakiko Fujita, Testuya Osato, Shiori Suzuki, Junko Ouchi, for technical support. Computational resources for genotype imputation were provided by the Tohoku Medical Megabank Organization supercomputer system. This research is (partially) supported by the Center of Innovation Program from Japan Science and Technology Agency, JST. The manuscript has been proof read by an English editing service (Enago Ltd., Tokyo, Japan).
Publisher Copyright:
Copyright: © 2017 Shiga et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
PY - 2017/12
Y1 - 2017/12
N2 - Purpose To test the genetic association between Japanese patients with primary open-angle glaucoma (POAG) and the previously reported POAG susceptibility loci and to perform genotype–phenotype analysis. Methods Genetic associations for 27 SNPs from 16 loci previously linked to POAG were assessed using genome-wide SNP data of the primary cohort (565 Japanese POAG patients and 1,104 controls). Reproducibility of the assessment was tested in 607 POAG cases and 455 controls (second cohort) with a targeted genotyping approach. For POAG-associated variants, a genotype–phenotype correlation study (additive, dominant, recessive model) was performed using the objective clinical data derived from 598 eyes of 598 POAG patients. Results Among 27 SNPs from 16 loci previously linked to POAG, genotypes for total of 20 SNPs in 13 loci were available for targeted association study. Among 8 SNPs in 3 loci that showed at least nominal association (P < 5.00E-02) in the primary cohort, a representative SNP for each loci (rs2157719 for CDKN2B-AS1, rs33912345 for SIX6, and rs9913911 for GAS7) were selected. For these SNPs the association was found significant in both the second cohort analysis and meta-analysis. The genotype–phenotype analysis revealed significant correlations between CDKN2B-AS1 (rs2157719) and decreased intraocular pressure (? = -6.89 mmHg, P = 1.70E-04; dominant model) after multiple corrections. In addition, nominal correlation was observed between CDKN2B-AS1 (rs2157719) and optic nerve head blood flow (? = -0.54 and -0.67 arbitrary units (AU), P = 2.00E-02 and 1.39E-02), between SIX6 (rs33912345) and decreased total peripapillary retinal nerve fiber layer thickness (? = -2.16 and -2.82 ?m, P = 4.68E-02 and 2.40E-02, additive and recessive model, respectively) and increased optic nerve head blood flow (? = 0.44 AU, P = 2.20E-02; additive model) and between GAS7 (rs9913911) and increased cup volume (? = 0.03 mm3, P = 4.60E-02) and mean cup depth (? = 0.03 mm3, P = 4.11E-02; additive model) and decreased pattern standard deviation (? = -0.87 dB, P = 2.44E-02; dominant model). Conclusion The association between SNPs near GAS7 and POAG was found in Japanese patients for the first time. Clinical characterization of the risk variants is an important step toward understanding the pathology of the disease and optimizing treatment of patients with POAG.
AB - Purpose To test the genetic association between Japanese patients with primary open-angle glaucoma (POAG) and the previously reported POAG susceptibility loci and to perform genotype–phenotype analysis. Methods Genetic associations for 27 SNPs from 16 loci previously linked to POAG were assessed using genome-wide SNP data of the primary cohort (565 Japanese POAG patients and 1,104 controls). Reproducibility of the assessment was tested in 607 POAG cases and 455 controls (second cohort) with a targeted genotyping approach. For POAG-associated variants, a genotype–phenotype correlation study (additive, dominant, recessive model) was performed using the objective clinical data derived from 598 eyes of 598 POAG patients. Results Among 27 SNPs from 16 loci previously linked to POAG, genotypes for total of 20 SNPs in 13 loci were available for targeted association study. Among 8 SNPs in 3 loci that showed at least nominal association (P < 5.00E-02) in the primary cohort, a representative SNP for each loci (rs2157719 for CDKN2B-AS1, rs33912345 for SIX6, and rs9913911 for GAS7) were selected. For these SNPs the association was found significant in both the second cohort analysis and meta-analysis. The genotype–phenotype analysis revealed significant correlations between CDKN2B-AS1 (rs2157719) and decreased intraocular pressure (? = -6.89 mmHg, P = 1.70E-04; dominant model) after multiple corrections. In addition, nominal correlation was observed between CDKN2B-AS1 (rs2157719) and optic nerve head blood flow (? = -0.54 and -0.67 arbitrary units (AU), P = 2.00E-02 and 1.39E-02), between SIX6 (rs33912345) and decreased total peripapillary retinal nerve fiber layer thickness (? = -2.16 and -2.82 ?m, P = 4.68E-02 and 2.40E-02, additive and recessive model, respectively) and increased optic nerve head blood flow (? = 0.44 AU, P = 2.20E-02; additive model) and between GAS7 (rs9913911) and increased cup volume (? = 0.03 mm3, P = 4.60E-02) and mean cup depth (? = 0.03 mm3, P = 4.11E-02; additive model) and decreased pattern standard deviation (? = -0.87 dB, P = 2.44E-02; dominant model). Conclusion The association between SNPs near GAS7 and POAG was found in Japanese patients for the first time. Clinical characterization of the risk variants is an important step toward understanding the pathology of the disease and optimizing treatment of patients with POAG.
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U2 - 10.1371/journal.pone.0186678
DO - 10.1371/journal.pone.0186678
M3 - Article
C2 - 29261660
AN - SCOPUS:85038886934
SN - 1932-6203
VL - 12
JO - PLoS One
JF - PLoS One
IS - 12
M1 - e0186678
ER -