METTL23 变异与正常张力青光眼患者。

IF 7.8 1区医学 Q1 OPHTHALMOLOGY

JAMA ophthalmology Pub Date : 2024-09-26 DOI:10.1001/jamaophthalmol.2024.3829

Todd E Scheetz,Mallory R Tollefson,Ben R Roos,Erin A Boese,Andrew E Pouw,Edwin M Stone,Michael J Schnieders,John H Fingert

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引用次数: 0

摘要

重要性这项研究证实并进一步确定了第四个基因 METTL23 的致病变体与常染色体显性正常张力性青光眼（NTG）有关。目的确定爱荷华州 NTG 患者队列中 METTL23 基因中青光眼致病变体的频率。设计、地点和参与者这项病例对照研究于 1997 年 1 月至 2024 年 1 月在爱荷华州的一家三级医疗中心进行，分析时间为 2023 年 1 月至 2024 年 1 月。爱荷华大学诊所招募了两组参与者：331 名 NTG 患者和 362 名无青光眼的对照组患者。有外伤史、类固醇使用史、色素分散综合征征兆、剥脱综合征或 MYOC、TBK1 或 OPTN 致病变异的患者也被排除在外。主要结果和测量指标与无青光眼的对照组相比，在 NTG 患者中检测到 METTL23 致病变异的富集。结果研究纳入了 331 名 NTG 患者（平均 [SD] 年龄 68.0 [11.7] 岁；228 [68.9%] 名女性和 103 [31.1%] 名男性）和 362 名无青光眼的对照组患者（平均 [SD] 年龄 64.5 [12.6] 岁；207 [57.2%] 名女性和 155 [42.8%] 名男性）。在 NTG 患者中检测到 5 例 4 个独特的 METTL23 致病变体。三个 METTL23 变异-p.Ala7Val、p.Pro22Arg 和 p.Arg63Trp-被判定为可能致病，并在 3 名 NTG 患者（0.91%）中检测到。然而，用突变负荷分析或逻辑回归评估所有检测到的变异时，它们在 NTG 患者中的频率在统计学上并不高于无青光眼的对照组（1.5% vs 2.5%；P = .27）。在一家三级医疗中心的 NTG 队列中，约有 1% 的 NTG 病例与致病变体有关，这一频率与其他已知的正常张力青光眼基因相似，包括视神经蛋白 (OPTN)、TANK 结合激酶 1 (TBK1) 和肌球蛋白 (MYOC)。研究结果表明，METTL23致病变体很可能参与了与在较低眼压下发生的青光眼有关的生物通路。

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METTL23 Variants and Patients With Normal-Tension Glaucoma.

Importance This research confirms and further establishes that pathogenic variants in a fourth gene, METTL23, are associated with autosomal dominant normal-tension glaucoma (NTG). Objective To determine the frequency of glaucoma-causing pathogenic variants in the METTL23 gene in a cohort of patients with NTG from Iowa. Design, Setting, and Participants This case-control study took place at a single tertiary care center in Iowa from January 1997 to January 2024, with analysis occurring between January 2023 and January 2024. Two groups of participants were enrolled from the University of Iowa clinics: 331 patients with NTG and 362 control individuals without glaucoma. Patients with a history of trauma; steroid use; stigmata of pigment dispersion syndrome; exfoliation syndrome; or pathogenic variants in MYOC, TBK1, or OPTN were also excluded. Main Outcomes and Measures Detection of an enrichment of METTL23 pathogenic variants in individuals with NTG compared with control individuals without glaucoma. Results The study included 331 patients with NTG (mean [SD] age, 68.0 [11.7] years; 228 [68.9%] female and 103 [31.1%] male) and 362 control individuals without glaucoma (mean [SD] age, 64.5 [12.6] years; 207 [57.2%] female and 155 [42.8%] male). There were 5 detected instances of 4 unique METTL23 pathogenic variants in patients with NTG. Three METTL23 variants-p.Ala7Val, p.Pro22Arg, and p.Arg63Trp-were judged to be likely pathogenic and were detected in 3 patients (0.91%) with NTG. However, when all detected variants were evaluated with either mutation burden analysis or logistic regression, their frequency was not statistically higher in individuals with NTG than in control individuals without glaucoma (1.5% vs 2.5%; P = .27). Conclusion and Relevance This investigation provides evidence that pathogenic variants in METTL23 are associated with NTG. Within an NTG cohort at a tertiary care center, pathogenic variants were associated with approximately 1% of NTG cases, a frequency similar to that of other known normal-tension glaucoma genes, including optineurin (OPTN), TANK-binding kinase 1 (TBK1), and myocilin (MYOC). The findings suggest that METTL23 pathogenic variants are likely involved in a biologic pathway that is associated with glaucoma that occurs at lower intraocular pressures.

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来源期刊

JAMA ophthalmology OPHTHALMOLOGY-

CiteScore

13.20

自引率

3.70%

发文量

340

期刊介绍： JAMA Ophthalmology, with a rich history of continuous publication since 1869, stands as a distinguished international, peer-reviewed journal dedicated to ophthalmology and visual science. In 2019, the journal proudly commemorated 150 years of uninterrupted service to the field. As a member of the esteemed JAMA Network, a consortium renowned for its peer-reviewed general medical and specialty publications, JAMA Ophthalmology upholds the highest standards of excellence in disseminating cutting-edge research and insights. Join us in celebrating our legacy and advancing the frontiers of ophthalmology and visual science.