玻璃体内药物治疗时代视网膜色素上皮撕裂:危险因素、发病机制、预后和治疗(美国眼科学会论文)。

David Sarraf, Anthony Joseph, Ehsan Rahimy
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引用次数: 0

摘要

目的:描述视网膜色素上皮(RPE)撕裂的危险因素、发病机制和预后,并证明我们的假设,即RPE撕裂后持续抗血管内皮生长因子(VEGF)治疗与改善长期视觉和解剖结果相关。方法:我们检索了一个包含10089例患者的数据库,并回顾性发现了56只眼的新生血管性年龄相关性黄斑变性(AMD)合并RPE撕裂的大病例系列,时间超过8年。将基线视力(VA)制成表格,并通过多模态成像分析RPE撕裂。评估随访VA、撕裂进展和纤维化严重程度,并与抗vegf注射次数相关。结果:56只眼的平均随访时间为42个月,基线时的平均logMAR VA为0.88 (Snellen VA 20/150), 3年内下降最小。LogMAR VA与抗vegf注射次数对比显示,越频繁和累积的注射与更好的VA相关(结论:抗vegf治疗后,由于1型脉络膜新生血管膜的进行性收缩,15%至20%的血管化色素上皮脱落(PED)可能发生RPE撕裂。持续监测RPE撕裂液的渗出性变化,以保证抗vegf治疗,可以稳定VA,改善解剖结果,减少纤维化,并降低发展为大致盲的终末期渗出性盘状疤痕的风险。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Retinal pigment epithelial tears in the era of intravitreal pharmacotherapy: risk factors, pathogenesis, prognosis and treatment (an American Ophthalmological Society thesis).

Retinal pigment epithelial tears in the era of intravitreal pharmacotherapy: risk factors, pathogenesis, prognosis and treatment (an American Ophthalmological Society thesis).

Retinal pigment epithelial tears in the era of intravitreal pharmacotherapy: risk factors, pathogenesis, prognosis and treatment (an American Ophthalmological Society thesis).

Retinal pigment epithelial tears in the era of intravitreal pharmacotherapy: risk factors, pathogenesis, prognosis and treatment (an American Ophthalmological Society thesis).

Purpose: To describe the risk factors, pathogenesis, and prognosis of retinal pigment epithelial (RPE) tears and to demonstrate our hypothesis that continued anti-vascular endothelial growth factor (VEGF) therapy after an RPE tear has occurred correlates with improved long-term visual and anatomical outcomes.

Methods: We searched a database of 10,089 patients and retrospectively identified a large case series of 56 eyes with neovascular age-related macular degeneration (AMD) complicated by an RPE tear over an 8-year period. Baseline visual acuity (VA) was tabulated and analysis of the RPE tear was performed with multimodal imaging. Follow-up VA, progression of the tear, and severity of fibrosis were evaluated, and each was correlated with number of anti-VEGF injections.

Results: Average follow-up for the 56 eyes was 42 months, and mean logMAR VA at baseline was 0.88 (Snellen VA 20/150) with minimal decline over 3 years. LogMAR VA plotted against number of anti-VEGF injections demonstrated that more frequent and cumulative injections correlated with better VA (P<.0001). A greater number of anti-VEGF injections was associated with minimal progression of the RPE tear, reduced fibrosis, and lower risk of a large, end-stage exudative disciform scar.

Conclusions: Fifteen to 20% of vascularized pigment epithelial detachments (PEDs) may develop RPE tears after anti-VEGF therapy due to progressive contraction of the type 1 choroidal neovascular membrane in a PED at risk. Continued monitoring of RPE tears for exudative changes warranting anti-VEGF therapy may stabilize VA, improve anatomical outcomes, reduce fibrosis, and decrease the risk of developing a large blinding end-stage exudative disciform scar.

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