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

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

作者信息

Sarraf David, Joseph Anthony, Rahimy Ehsan

机构信息

Jules Stein Eye Institute, David Geffen School of Medicine at UCLA, Los Angeles, California.

出版信息

Trans Am Ophthalmol Soc. 2014 Jul;112:142-59.

Abstract

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.

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撕裂发生后继续抗血管内皮生长因子(VEGF)治疗与改善长期视力和解剖学结果相关。

方法

我们检索了一个包含10089例患者的数据库,并回顾性确定了一个大型病例系列,其中56只眼患有新生血管性年龄相关性黄斑变性(AMD)并在8年期间并发RPE撕裂。记录基线视力(VA),并使用多模态成像对RPE撕裂进行分析。评估随访VA、撕裂进展和纤维化严重程度,并将每一项与抗VEGF注射次数相关联。

结果

56只眼的平均随访时间为42个月,基线时平均logMAR VA为0.88(Snellen视力20/150),3年内下降最小。将logMAR VA与抗VEGF注射次数作图显示,更频繁和累积的注射与更好的VA相关(P<0.0001)。更多的抗VEGF注射与RPE撕裂的最小进展、纤维化减少以及大的终末期渗出性盘状瘢痕风险降低相关。

结论

15%至20%的血管化色素上皮脱离(PED)在抗VEGF治疗后可能由于PED中1型脉络膜新生血管膜的渐进性收缩而发生RPE撕裂。持续监测RPE撕裂的渗出性变化以确定是否需要抗VEGF治疗可能会稳定VA、改善解剖学结果、减少纤维化并降低发生大的致盲性终末期渗出性盘状瘢痕的风险。

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