4.4 Article

Prevalence of MYOC risk variants for glaucoma in different populations

期刊

ACTA OPHTHALMOLOGICA
卷 99, 期 7, 页码 E1090-E1097

出版社

WILEY
DOI: 10.1111/aos.14738

关键词

open-angle glaucoma; juvenile glaucoma; JOAG; POAG; myocilin; MYOC

资金

  1. Glaukooma Tukisaatio Lux Foundation
  2. Evald and Hilda Nissi Foundation

向作者/读者索取更多资源

Pathogenic variants in the MYOC gene show population-specific prevalence, with certain variants being more common in East and South Asia. The study highlights allelic heterogeneity of MYOC variants in open-angle glaucoma, suggesting doubt on their status as monogenic disease-causing variants in some populations. The carrier frequencies of these variants vary in different subpopulations, implying a complex genetic landscape for glaucoma risk factors.
Purpose To assess the clinical relevance of myocilin (MYOC) gene variants as risk factors for glaucoma in literature and to estimate their prevalence in different populations. Methods We reviewed the literature for published MYOC variants in glaucoma patients and estimated their prevalence in general population using gnomAD and BRAVO databases. We used several bioinformatics tools and the criteria of the American College of Medical Genetics and Genomics (ACMG) to assess the pathogenicity of the variants. We evaluated the carrier frequency of the variants in gnomAD, including its subpopulations. Results We found 13 missense and 5 loss-of-function (LOF) reported variants in MYOC that were both probable pathogenic or risk variants and listed in gnomAD. Six likely pathogenic missense variants were p.(Cys25Arg), p.(Gln48His), p.(Gly326Ser), p.(Thr353Ile), p.(Thr377Met) and p.(Gly399Val). They were most prevalent in East and South Asia (frequency, 0.92% and 0.81%, respectively). The most common missense variants were p.(Thr353Ile) (0.91% in East Asia) and p.(Gln48His) (0.79% in South Asia). Five LOF variants were p.(Arg46Ter), p.(Arg91Ter), p.(Arg272Ter), p.(Gln368Ter) and p.(Tyr453MetfsTer11). We considered these glaucoma risk variants. They were most prevalent in the East Asian and the Finnish population (0.93% and 0.33%, respectively). Conclusion Pathogenic MYOC variants appear to be population-associated. Our results highlight allelic heterogeneity of MYOC variants in open-angle glaucoma. Many of the probable pathogenic variants are over-represented in some of the populations causing doubt of their status as monogenic disease-causing variants.

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