Heritable Risk and Protective Genetic Components of Glaucoma Medication Non-Adherence

Barr, Julie L.; Feehan, Michael; Tak, Casey; Owen, Leah A.; Finley, Robert C.; Cromwell, Parker A.; Lillvis, John H.; Hicks, Patrice M.; Au, Elizabeth; Farkas, Michael H.; Weiner, Asher; Reynolds, Andrew L.; Sieminski, Sandra; Sherva, Richard; Munger, Mark A.; Brilliant, Murray H.; DeAngelis, Margaret M.

doi:10.3390/ijms24065636

Cited by 3 publications

(1 citation statement)

References 56 publications

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“…This may underlie clinically observed differences in ROP development, which are also represented in our cohort which demonstrates African American ROP prevalence of 43% compared to 52% and 67% for European Ancestry and Hispanic populations respectively. Replication of this study using a larger and more diverse population is needed to validate these findings, particularly with regard to differences in genetic ROP risk relative to ethnicity and race 80 – 82 . In summary and to the best of our knowledge, we report the largest ROP GWAS to date, identifying a novel GWS locus at GLI3 with possible functional relevance supporting translation toward improved patient outcomes for at-risk preterm infants.…”

Section: Discussionmentioning

confidence: 93%

Genome-wide association identifies novel ROP risk loci in a multiethnic cohort

Li,

Owen,

Taylor

et al. 2024

Commun Biol

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We conducted a genome-wide association study (GWAS) in a multiethnic cohort of 920 at-risk infants for retinopathy of prematurity (ROP), a major cause of childhood blindness, identifying 1 locus at genome-wide significance level (p < 5×10-8) and 9 with significance of p < 5×10-6 for ROP ≥ stage 3. The most significant locus, rs2058019, reached genome-wide significance within the full multiethnic cohort (p = 4.96×10-9); Hispanic and European Ancestry infants driving the association. The lead single nucleotide polymorphism (SNP) falls in an intronic region within the Glioma-associated oncogene family zinc finger 3 (GLI3) gene. Relevance for GLI3 and other top-associated genes to human ocular disease was substantiated through in-silico extension analyses, genetic risk score analysis and expression profiling in human donor eye tissues. Thus, we identify a novel locus at GLI3 with relevance to retinal biology, supporting genetic susceptibilities for ROP risk with possible variability by race and ethnicity.

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Section: Discussionmentioning

confidence: 93%

Genome-wide association identifies novel ROP risk loci in a multiethnic cohort

Li,

Owen,

Taylor

et al. 2024

Commun Biol

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Genome-wide association identifies novel ROP risk loci in a multi-ethnic cohort

Rotter¹,

Owen

et al. 2023

Preprint

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We conducted a genome-wide association study (GWAS) in a multiethnic cohort of 920 at-risk infants for retinopathy of prematurity (ROP), a major cause of childhood blindness, identifying 2 loci at genome-wide significance level (p<5×10-8) and 7 at suggestive significance (p<5×10-6) for ROP ≥ stage 3. The most significant locus, rs2058019, reached genome-wide significance within the full multiethnic cohort (p= 4.96×10-9); Hispanic and Caucasian infants driving the association. The lead single nucleotide polymorphism (SNP) falls in an intronic region within the Glioma-associated oncogene family zinc finger 3 (GLI3) gene. Relevance for GLI3 and other top-associated genes to human ocular disease was substantiated through in-silico extension analyses, genetic risk score analysis and expression profiling in human donor eye tissues. Thus, we report the largest ROP GWAS to date, identifying a novel locus at GLI3 with relevance to retinal biology supporting genetic susceptibilities for ROP risk with possible variability by race and ethnicity.

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Patterns of Gene Expression, Splicing, and Allele-Specific Expression Vary among Macular Tissues and Clinical Stages of Age-Related Macular Degeneration

Shwani,

Zhang,

Owen

et al. 2023

Cells

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Age-related macular degeneration (AMD) is a leading cause of blindness, and elucidating its underlying disease mechanisms is vital to the development of appropriate therapeutics. We identified differentially expressed genes (DEGs) and differentially spliced genes (DSGs) across the clinical stages of AMD in disease-affected tissue, the macular retina pigment epithelium (RPE)/choroid and the macular neural retina within the same eye. We utilized 27 deeply phenotyped donor eyes (recovered within a 6 h postmortem interval time) from Caucasian donors (60–94 years) using a standardized published protocol. Significant findings were then validated in an independent set of well-characterized donor eyes (n = 85). There was limited overlap between DEGs and DSGs, suggesting distinct mechanisms at play in AMD pathophysiology. A greater number of previously reported AMD loci overlapped with DSGs compared to DEGs between disease states, and no DEG overlap with previously reported loci was found in the macular retina between disease states. Additionally, we explored allele-specific expression (ASE) in coding regions of previously reported AMD risk loci, uncovering a significant imbalance in C3 rs2230199 and CFH rs1061170 in the macular RPE/choroid for normal eyes and intermediate AMD (iAMD), and for CFH rs1061147 in the macular RPE/choroid for normal eyes and iAMD, and separately neovascular AMD (NEO). Only significant DEGs/DSGs from the macular RPE/choroid were found to overlap between disease states. STAT1, validated between the iAMD vs. normal comparison, and AGTPBP1, BBS5, CERKL, FGFBP2, KIFC3, RORα, and ZNF292, validated between the NEO vs. normal comparison, revealed an intricate regulatory network with transcription factors and miRNAs identifying potential upstream and downstream regulators. Findings regarding the complement genes C3 and CFH suggest that coding variants at these loci may influence AMD development via an imbalance of gene expression in a tissue-specific manner. Our study provides crucial insights into the multifaceted genomic underpinnings of AMD (i.e., tissue-specific gene expression changes, potential splice variation, and allelic imbalance), which may open new avenues for AMD diagnostics and therapies specific to iAMD and NEO.

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Heritable Risk and Protective Genetic Components of Glaucoma Medication Non-Adherence

Cited by 3 publications

References 56 publications

Genome-wide association identifies novel ROP risk loci in a multiethnic cohort

Genome-wide association identifies novel ROP risk loci in a multiethnic cohort

Genome-wide association identifies novel ROP risk loci in a multi-ethnic cohort

Patterns of Gene Expression, Splicing, and Allele-Specific Expression Vary among Macular Tissues and Clinical Stages of Age-Related Macular Degeneration

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