The protective variant rs7173049 at LOXL1 locus impacts on retinoic acid signaling pathway in pseudoexfoliation syndrome

Berner, Daniel; Hoja, Ursula; Zenkel, Matthias; Ross, James J.; Uebe, Steffen; Paoli, Daniela; Frezzotti, Paolo; Rautenbach, Robyn M.; Ziskind, Ari; Williams, Susan E.; Carmichael, Trevor; Ramsay, Michèle; Topouzis, Fotis; Chatzikyriakidou, A.; Lambropoulos, Alexandros; Sundaresan, Periasamy; Ayub, Humaira; Akhtar, Farah; Qamar, Raheel; Zenteno, Juan Carlos; Cruz‐Aguilar, Marisa; Astakhov, Yury S; Dubina, Michael; Wiggs, Janey L.; Ozaki, Mineo; Kruse, Friedrich E.; Aung, Tin; Reis, André; Khor, Chiea Chuen; Pasutto, Francesca; Schlötzer‐Schrehardt, Ursula

doi:10.1093/hmg/ddz075

Cited by 24 publications

(30 citation statements)

References 86 publications

(108 reference statements)

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“…Protective function of rs7173049‐G allele is believed to be through the upregulation of STRA6 , which is involved in cellular uptake of vitamin A and was shown to be significantly downregulated in XFS eyes (Berner et al. ). Another deep sequencing analysis has been conducted across LOXL1 locus in a collection of 5570 XFS cases and 6279 controls drawn from nine countries.…”

Section: Genetic Factors: Loxl1mentioning

confidence: 99%

“…A common non-coding variant rs7173049A>G was found downstream of LOXL1, suggested to be associated with decreased risk of XFS in different ethnic groups, where the minor allele G was shown to be constantly enriched in controls. Protective function of rs7173049-G allele is believed to be through the upregulation of STRA6, which is involved in cellular uptake of vitamin A and was shown to be significantly downregulated in XFS eyes (Berner et al 2019). Another deep sequencing analysis has been conducted across LOXL1 locus in a collection of 5570 XFS cases and 6279 controls drawn from nine countries.…”

Section: Genetic Factors: Loxl1mentioning

confidence: 99%

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Recent advances in risk factors associated with ocular exfoliation syndrome

Sharaf

Damji

Unsworth

2019

Acta Ophthalmologica

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Exfoliation syndrome is generally considered a progressive age‐related systemic disorder of the extracellular matrix, which is clinically characterized through the observation of flaky white aggregates on ocular tissues. Exfoliation syndrome is directly linked to exfoliative glaucoma in elderly patients, where it is known as the most common identifiable cause of open‐angle glaucoma. Despite the identification of various risk factors associated with exfoliation syndrome, the exact pathogenesis of this syndrome has not been fully elucidated. There is a growing number of genome‐wide association studies in different populations around the world to identify genetic factors underlying exfoliation syndrome. Besides variants in LOXL1 and CACNA1A genes, new loci have been recently identified which are believed to be associated with exfoliation syndrome. Among different genetic factors, functional variants might help to better understand mechanisms underlying this systemic disorder. Besides genetic factors, epigenetic regulation of different gene expression patterns has been thought to play a role in its pathogenesis. Other factors have been also considered to be involved in the development of exfoliation syndrome at cellular organelles level where mitochondrial impairment and autophagy dysfunction have been suggested in relation to exfoliation syndrome. This review addresses the most recent findings on genetic factors as well as cellular and molecular mechanisms involved in both the development and progression of exfoliation syndrome.

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Section: Genetic Factors: Loxl1mentioning

confidence: 99%

Section: Genetic Factors: Loxl1mentioning

confidence: 99%

Recent advances in risk factors associated with ocular exfoliation syndrome

Sharaf

Damji

Unsworth

2019

Acta Ophthalmologica

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“…25 These data indicate that dysregulation of STRA6 and impaired retinoid metabolism are involved in the pathophysiology of XFS syndrome. Retinoic acid, the active metabolite involved in the signaling pathway implicated by Berner et al 25 in XFS through regulation of ISLR2, STRA6 and LOXL1, has been shown to control critical checkpoints in inflammation and to promote an inflammatory environment. [111][112][113] In summary, our analysis of predicted gene expression and extensive functional analysis in eye tissue prioritized six genes in association with XFS.…”

Section: Limitations Of the Studymentioning

confidence: 84%

“…Some of these non-coding variants regulate expressions of the sentinel LOXL1 and the neighboring STRA6 gene. 7,25,26 After considering all the reports on genetic architecture of XFS to date, we hypothesize that analysis of the contribution of the genetically-determined component of gene expression to XFS risk can provide a powerful method to elucidate genes involved in XFS. We used a genebased method, PrediXcan 27 , implemented on GWAS summary statistics (Summary PrediXcan; S-PrediXcan) 28 to identify genetically determined gene expression traits associated with disease risk.…”

Section: Introductionmentioning

confidence: 99%

Analysis of Genetically Determined Gene Expression Suggests Role of Inflammatory Processes in Etiology of Exfoliation Syndrome

Hirbo

Pasutto

Gamazon

et al. 2020

Preprint

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Exfoliation syndrome (XFS) is an age-related systemic disorder characterized by excessive production and progressive accumulation of abnormal extracellular material, with pathognomonic ocular manifestations. It is the most common cause of secondary glaucoma, resulting in widespread global blindness. We performed Transcriptomic Wide Association Studies using PrediXcan models trained in 48 GTEx tissues to identify genetically-determined gene expression changes associated with XFS risk, leveraging on results from a global GWAS that included 123,457 individuals from 24 countries. Twenty-eight genes in the chr15q22-25 region showed statistically significant associations in both single-tissue and multi-tissue analysis. Reduced models for these genes that excluded variants in LD with the known LOXL1 signal showed genome-wide significant association signals in nine genes, independently of LOXL1. Out of these ten genes, mRNA transcript levels for ARID3B, CD276, LOXL1, NEO1, SCAMP2, and UBL7 were significantly decreased in iris tissues from XFS patients compared to control samples. Genes with genetically determined expression changes in XFS were significantly enriched for genes associated with inflammatory conditions. We further explored the health consequences of high susceptibility to XFS using a large electronic health record and observed a higher incidence of XFS comorbidity with inflammatory and connective tissue diseases. Our results implicate a role for connective tissues and inflammation in the etiology of XFS. Targeting the inflammatory pathway may be a potential therapeutic option to reduce progression in XFS.

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“…Some of these non-coding variants regulate expressions of the sentinel LOXL1 and the neighboring STRA6 gene. 7,25,26 After considering all the reports on genetic architecture of XFS to date, we hypothesize that analysis of the contribution of the genetically-determined component of gene expression to XFS risk can provide a powerful method to elucidate genes involved in XFS. We used a genebased TWAS method, PrediXcan 27 , implemented on GWAS summary statistics (Summary PrediXcan; S-PrediXcan) 28 to identify genetically determined gene expression traits associated with disease risk.…”

Section: Introductionmentioning

confidence: 99%

Analysis of Genetically Determined Gene Expression Suggests Role of Inflammatory Processes in Exfoliation Syndrome

Hirbo¹,

Pasutto

Gamazon

et al. 2020

Preprint

Self Cite

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Exfoliation syndrome (XFS) is an age-related systemic disorder characterized by excessive production and progressive accumulation of abnormal extracellular material, with pathognomonic ocular manifestations. It is the most common cause of secondary glaucoma, resulting in widespread global blindness. We performed Transcriptomic Wide Association Studies (TWAS) using PrediXcan models trained in 48 GTEx tissues to identify genetically- determined gene expression changes associated with XFS risk, leveraging on results from a global GWAS that included 123,457 individuals from 24 countries. We observed twenty-eight genes in a three-Megabase chr15q22-25 region that showed statistically significant associations, which were further whittled down to ten genes after additional statistical validations. In experimental analysist of these ten genes, mRNA transcript levels for ARID3B, CD276, LOXL1, NEO1, SCAMP2, and UBL7 were significantly decreased in iris tissues from XFS patients compared to control samples. Genes with genetically determined expression changes in XFS were significantly enriched for genes associated with inflammatory conditions. We further explored the health consequences of high susceptibility to XFS using a large electronic health record and observed a higher incidence of XFS comorbidity with inflammatory and connective tissue diseases. Our results implicate a role for connective tissues and inflammation in the etiology of XFS. Targeting the inflammatory pathway may be a potential therapeutic option to reduce progression in XFS.

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The protective variant rs7173049 at LOXL1 locus impacts on retinoic acid signaling pathway in pseudoexfoliation syndrome

Cited by 24 publications

References 86 publications

Recent advances in risk factors associated with ocular exfoliation syndrome

Recent advances in risk factors associated with ocular exfoliation syndrome

Analysis of Genetically Determined Gene Expression Suggests Role of Inflammatory Processes in Etiology of Exfoliation Syndrome

Analysis of Genetically Determined Gene Expression Suggests Role of Inflammatory Processes in Exfoliation Syndrome

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