英国生物银行中载脂蛋白E E4等位基因与青光眼诊断年龄之间的女性特异性关联
Female-Specific Association between the Apolipoprotein E E4 Allele and Age at Diagnosis of Glaucoma in UK Biobank.
作者信息
Shi Yan, Hu Junming, Liu William, Qiu Wei Qiao, He Xinyue, Zhang Miao, Gao Yan, Zhang Xiaoling, Fan Zhigang
机构信息
Beijing Tongren Eye Center Research Ward, Beijing Tongren Hospital, Beijing Institute of Ophthalmology, Beijing Ophthalmology & Visual Sciences Key Laboratory, Capital Medical University, Beijing, China; Departments of Medicine (Biomedical Genetics), Boston University School of Medicine, Boston, Massachusetts.
Departments of Medicine (Biomedical Genetics), Boston University School of Medicine, Boston, Massachusetts.
出版信息
Ophthalmol Glaucoma. 2025 Jan-Feb;8(1):53-62. doi: 10.1016/j.ogla.2024.07.009. Epub 2024 Aug 7.
OBJECTIVE
To explore the impact of the apolipoprotein E (APOE) E4 allele in the gender-specific aging process in glaucoma by illustrating the interaction between risk factors, including the APOE E4 allele, gender, and intraocular pressure (IOP), for age at diagnosis (AAD) of glaucoma.
DESIGN
A cross-sectional study included UK Biobank participants with complete data (2006-2010) for analysis. Data were analyzed in December 2023.
PARTICIPANTS
Two thousand two hundred thirty-six glaucoma patients and 103 232 controls.
METHODS
We evaluated multivariable-adjusted associations of AAD of glaucoma, APOE E4 allele (0: absence; 1: presence), and IOP using linear mixed model (LMM) analyses across groups stratified by AAD of mean age of menopause (50 years) and gender.
MAIN OUTCOMES MEASURES
Age at diagnosis of glaucoma, APOE E4 allele, and IOP.
RESULTS
Patients with glaucoma were older and had a higher percentage of males and a higher mean IOP compared to controls (all P < 0.001). Further stratifying the patients with glaucoma by AAD of 50 and gender, lower IOP (model 1 adjusted by age, β = -0.096 ± 0.041, P = 0.019), and positive APOE E4 allele (model 2 adjusted by age and IOP, β = 1.093 ± 0.488, P = 0.026) were associated with an older AAD in females with an AAD <50 years under univariate LMM. In multivariate LMM adjusted by age (model 3), the effect size of both factors increased in the multivariate model as the beta-value increased (β = -0.111 ± 0.040, P = 0.007; β = 1.235 ± 0.485, P = 0.012) (model 1 vs. model 3: P = 0.011). In females with an AAD ≥50 years, only positive APOE E4 allele (adjusted by age and IOP, β = -1.121 ± 0.412, P = 0.007) was associated with a younger AAD. In males, only higher IOP was associated with an older AAD in those with an AAD ≥50 years (β = 0.088 ± 0.032, P = 0.006).
CONCLUSIONS
Apolipoprotein E E4 allele may initially delay and later accelerate the development of glaucoma in females around the transition period of 50 years, which is the mean age of menopause, and importantly, this is independent of IOP. Understanding the specific transition states and modifiable factors within each age phase is crucial for developing interventions or strategies that promote healthy aging.
FINANCIAL DISCLOSURES
Proprietary or commercial disclosure may be found in the Footnotes and Disclosures at the end of this article.
目的
通过阐述包括载脂蛋白E(APOE)E4等位基因、性别和眼压(IOP)在内的危险因素之间的相互作用,探讨APOE E4等位基因在青光眼性别特异性衰老过程中的影响,以确定青光眼的诊断年龄(AAD)。
设计
一项横断面研究纳入了英国生物银行中具有完整数据(2006 - 2010年)以供分析的参与者。数据于2023年12月进行分析。
参与者
2236例青光眼患者和103232例对照。
方法
我们使用线性混合模型(LMM)分析,在按绝经平均年龄(50岁)和性别分层的组中,评估青光眼的AAD、APOE E4等位基因(0:不存在;1:存在)和IOP的多变量调整关联。
主要观察指标
青光眼的诊断年龄、APOE E4等位基因和IOP。
结果
与对照组相比,青光眼患者年龄更大,男性比例更高,平均IOP更高(所有P < 0.001)。按AAD为50岁和性别对青光眼患者进一步分层,在单变量LMM中,较低的IOP(模型1经年龄调整,β = -0.096 ± 0.041,P = 0.019)和APOE E4等位基因阳性(模型2经年龄和IOP调整,β = 1.093 ± 0.488,P = 0.026)与AAD < 50岁的女性中AAD较大有关。在经年龄调整的多变量LMM(模型3)中,随着β值增加,两个因素在多变量模型中的效应大小均增加(β = -0.111 ± 0.040,P = 0.007;β = 1.235 ± 0.485,P = 0.012)(模型1与模型3:P = 0.011)。在AAD≥50岁的女性中,只有APOE E4等位基因阳性(经年龄和IOP调整,β = -1.121 ± 0.412,P = 0.007)与AAD较小有关。在男性中,只有较高的IOP与AAD≥50岁的男性中AAD较大有关(β = 0.088 ± 0.032,P = 0.006)。
结论
载脂蛋白E E4等位基因可能在50岁左右(绝经平均年龄)的女性过渡期最初延迟并随后加速青光眼的发展,重要的是,这与IOP无关。了解每个年龄阶段的特定过渡状态和可改变因素对于制定促进健康衰老的干预措施或策略至关重要。
财务披露
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