Risk of Adverse Systemic Events in Retinal Vein Occlusion.

IF 4.4 Q1 OPHTHALMOLOGY

Ophthalmology. Retina Pub Date : 2025-05-09 DOI:10.1016/j.oret.2025.05.005

Emily A Albrecht, Priya Shukla, Alison H Zhao, Jonathan C Markle, Christopher M Maatouk, Rishi P Singh, Katherine E Talcott

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Abstract

Purpose: Conflicting data exists on whether central and branch retinal vein occlusion (CRVO and BRVO) are linked to systemic adverse events. This study examines this association using the TriNetX US Collaborative Network, encompassing more than 110 million patients.

Design: Retrospective population-based cohort design.

Subjects and controls: CRVO and BRVO cohorts were compared to control cataract cohorts and between high and low-intensity treatment defined by ≥10 compared to ≤5 anti-vascular endothelial growth factor (anti-VEGF) injections.

Methods: This study used deidentified data from a national database (2006-2024), using International Classification of Diseases 10 codes for CRVO and BRVO. Patients were propensity score matched on demographics, medications, and comorbidities. Risk ratios were generated for systemic events in CRVO and BRVO patients compared to controls, and between patients with high and low-intensity treatment.

Main outcome measures: Risk ratios (RRs) and 95% confidence intervals (CIs) of death, myocardial infarction (MI), hemorrhagic stroke, ischemic stroke, and carotid disease.

Results: CRVO was associated with increased risk of death (RR 1.30; 95% CI 1.26-1.35), MI (RR 1.24; 1.16-1.32), hemorrhagic stroke (RR 1.35; 1.21-1.51), ischemic stroke (RR 1.49; 1.4-1.59), and carotid disease (RR 1.69; 1.59-1.79). BRVO was associated with increased risk of death (RR 1.27; 1.23-1.32), MI (RR 1.39; 1.30-1.49), hemorrhagic stroke (RR 1.57; 1.41-1.75), ischemic stroke (RR 1.66; 1.56-1.77), and carotid disease (RR 1.67; 1.57-1.77). CRVO with high-intensity treatment was associated with increased risk of MI (RR 1.47; 1.12-1.93) compared to low-intensity CRVO treatment, but there were no significant differences in risk of death (RR 0.98; 0.86-1.11), hemorrhagic stroke (RR 1.00; 0.63-1.58), ischemic stroke (RR 1.31; 1.03-1.66), or carotid disease (RR 1.34; 1.06-1.70). For BRVO with high compared to low-intensity treatment, no significant differences in rates of death (RR 1.12; 0.96-1.31), MI (RR 1.30; 0.93-1.81), hemorrhagic stroke (RR 0.96; 0.60-1.53), ischemic stroke (RR 1.05; 0.80-1.38), or carotid disease (RR 1.17; 0.85-1.60) were identified.

Conclusions: CRVO and BRVO are associated with increased risk of death, MI, hemorrhagic stroke, ischemic stroke, and carotid disease. High-intensity treatment of CRVO may be associated with increased risk of MI. These results from this dataset demonstrate the importance of systemic evaluation after RVO.

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视网膜静脉阻塞中不良系统事件的风险。

目的：关于视网膜中央和分支静脉阻塞（CRVO和BRVO）是否与全身不良事件相关的数据存在矛盾。本研究使用TriNetX美国合作网络（包括1.1亿多名患者）来检验这种关联。设计：基于人群的回顾性队列设计。受试者和对照组：将CRVO和BRVO队列与对照白内障队列进行比较，并将高强度治疗与低强度治疗（≥10次与≤5次注射抗血管内皮生长因子（anti-VEGF））进行比较。方法：本研究使用来自国家数据库（2006-2024）的未识别数据，使用国际疾病分类10 CRVO和BRVO代码。患者在人口统计学、药物和合并症方面的倾向评分相匹配。CRVO和BRVO患者与对照组相比，以及高强度和低强度治疗患者之间的系统性事件风险比。主要结局指标：死亡、心肌梗死、出血性卒中、缺血性卒中和颈动脉疾病的风险比（rr）和95%置信区间（CIs）。结果：CRVO与死亡风险增加相关(RR 1.30；95% ci 1.26-1.35), mi (rr 1.24；1.16-1.32)，出血性中风(RR 1.35；1.21-1.51)，缺血性卒中(RR 1.49；1.4-1.59)，颈动脉疾病(RR 1.69；1.59 - -1.79)。BRVO与死亡风险增加相关(RR 1.27；1.23-1.32), mi (rr 1.39；1.30-1.49)，出血性中风(RR 1.57；1.41-1.75)，缺血性卒中(RR 1.66；1.56-1.77)，颈动脉疾病(RR 1.67；1.57 - -1.77)。高强度治疗的CRVO与心肌梗死风险增加相关(RR 1.47；1.12-1.93)与低强度CRVO治疗相比，但死亡风险无显著差异(RR 0.98；出血性中风(RR 1.00；0.63-1.58)，缺血性卒中(RR 1.31；1.03-1.66)或颈动脉疾病(RR 1.34；1.06 - -1.70)。对于BRVO，高强度治疗与低强度治疗相比，死亡率无显著差异(RR 1.12；0.96-1.31), mi (rr 1.30；出血性卒中(RR 0.96；0.60-1.53)，缺血性卒中(RR 1.05；0.80-1.38)或颈动脉疾病(RR 1.17；0.85-1.60)。结论：CRVO和BRVO与死亡、心肌梗死、出血性卒中、缺血性卒中和颈动脉疾病的风险增加相关。CRVO的高强度治疗可能与心肌梗死风险增加有关。这些数据集的结果表明了RVO后系统评估的重要性。

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