Genetic Associations of Primary Angle-Closure Disease: A Systematic Review and Meta-Analysis

Yu Jing Liang; Yu Yao Wang; Shi Song Rong; Zhen Ji Chen; Shu Ying Chen; Jenson A Tham; Poemen P Chan; Jason C Yam; Janey L Wiggs; Chi Pui Pang; Clement C Tham; Li Jia Chen

doi:10.1001/jamaophthalmol.2024.0363

Genetic Associations of Primary Angle-Closure Disease: A Systematic Review and Meta-Analysis

JAMA Ophthalmol. 2024 Mar 28;142(5):437-444. doi: 10.1001/jamaophthalmol.2024.0363. Online ahead of print.

Authors

Yu Jing Liang¹, Yu Yao Wang¹, Shi Song Rong², Zhen Ji Chen¹, Shu Ying Chen¹, Jenson A Tham¹, Poemen P Chan^{1

3}, Jason C Yam^{1

3}, Janey L Wiggs², Chi Pui Pang¹, Clement C Tham^{1

3

4}, Li Jia Chen^{1

3

4}

Affiliations

¹ Department of Ophthalmology and Visual Sciences, The Chinese University of Hong Kong, Hong Kong, China.
² Department of Ophthalmology, Mass Eye and Ear, Mass General Brigham, Boston, Massachusetts.
³ Hong Kong Eye Hospital, Hong Kong, China.
⁴ Department of Ophthalmology and Visual Sciences, Prince of Wales Hospital, Hong Kong, China.

PMID: 38546604
PMCID: PMC10979365 (available on 2025-03-28)
DOI: 10.1001/jamaophthalmol.2024.0363

Abstract

Importance: Effects of genetic variants on primary angle-closure disease remained uncertain.

Objective: To systematically review the associations of common single-nucleotide variants (SNVs) and rare coding variants with primary angle-closure disease, its subtypes (including primary angle-closure glaucoma, primary angle-closure suspect, and primary angle-closure) and progression.

Data sources: Eligible studies from PubMed, Embase, and Web of Science were retrieved up to April 3, 2023. SNV information was extracted from eligible reports and 2 genome-wide association studies summary statistics, UK BioBank and FinnGen.

Study selection: Studies providing analyzable genotype or allele data in a case-control design for primary angle-closure disease association and longitudinal case-only design for primary angle-closure disease progression.

Data extraction and synthesis: PRISMA guidelines were used for literature screening and the Newcastle Ottawa Scale for data quality assessment. Pooled effect size with 95% CIs of SNV associations were calculated using fixed- or random-effect models according to I2 statistics.

Main outcomes and measures: SNVs reported in 2 or more studies were meta-analyzed to generate pooled odds ratios and P values. Common and rare coding variants from single reports were summarized.

Results: Sixty-nine citations were eligible for meta-analysis on overall primary angle-closure disease, involving 206 SNVs in 64 genes or loci. Seventeen SNVs in 15 genes or loci showed associations with primary angle-closure disease, and 15 SNVs in 13 genes or loci showed associations with primary angle-closure glaucoma. Two SNVs, ABCA1 rs2422493 and ZNRF3 rs3178915, were associated only with primary angle-closure disease. Two SNVs, PCMTD1-ST18 rs1015213 and COL11A1 rs3753841, were associated with primary angle-closure suspect, and 1 SNV, MMP9 rs3918249, was associated with primary angle-closure. This systematic review and meta-analysis newly confirmed 7 genes or loci associated with primary angle-closure glaucoma: ATOH7, CALCRL, FBN1, IL6, LOXL1, MMP19, and VAV3. Common and rare coding variants in 16 genes or loci that have been associated with primary angle-closure disease were cataloged. Stratification analysis revealed different primary angle-closure disease-associated genes in different ethnic populations. Only 1 study regarding the genetic association of primary angle-closure glaucoma progression was identified.

Conclusions and relevance: This study revealed the genetic complexity of primary angle-closure disease, involving common SNVs and rare coding variants in more than 30 genes or loci, with ethnic and phenotypic diversities. Further replication, genotype-phenotype correlation, and pathway analyses are warranted.