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在息肉样脉络膜血管病变的抗血管内皮生长因子治疗期间脉络膜状况的动态变化。

Dynamic changes in choroidal conditions during anti-vascular endothelial growth factor therapy in polypoidal choroidal vasculopathy.

机构信息

Laboratory of Retinal Cell Biology, Keio University, School of Medicine, Tokyo, Japan.

Department of Ophthalmology, Keio University, School of Medicine, Tokyo, Japan.

出版信息

Sci Rep. 2019 Aug 6;9(1):11389. doi: 10.1038/s41598-019-47738-9.

Abstract

We defined the relationships between initial choroidal conditions and their dynamics and exudative changes during anti-vascular endothelial growth factor (anti-VEGF) therapy in polypoidal choroidal vasculopathy (PCV). One hundred treatment-naïve eyes of 100 patients with PCV treated for 24 months at Keio University Hospital with intravitreal ranibizumab or aflibercept monotherapy (three injections and PRN thereafter) were retrospectively analyzed. Wet macula risk after three induction injections, which affected visual prognosis, was predicted by initial pachyvessels in the choroid (foveal greatest vertical choroidal vessel diameter [CVD] ≥180 μm) and pachychoroid (central choroidal thickness [CCT] ≥220 μm) recorded by optical coherence tomography. The risk for recurrent exudative change was greater in the pachyvessel groups irrespective of presence or absence of pachychoroid. Mean CVD and CCT decreased with anti-VEGF therapy when achieving a dry macula, suggesting that exudative changes are regulated by VEGF. Mean CVD and CCT at remission were greater in patients with initial pachyvessels and pachychoroid than in those without; the basal levels of CVD and CCT most likely represent VEGF-unrelated conditions. CVD increase preceded CCT increase and recurrent exudative changes, suggesting that the VEGF-related CVD increase may regulate CCT and exudative change; and that CVD may be a biomarker of exudative change.

摘要

我们定义了初始脉络膜条件与其动力学以及抗血管内皮生长因子(抗-VEGF)治疗期间息肉样脉络膜血管病变(PCV)渗出性变化之间的关系。在庆应义塾大学医院,对 100 例未经治疗的 PCV 患者的 100 只眼进行了回顾性分析,这些患者接受了玻璃体内雷珠单抗或阿柏西普单药治疗(此后每 3 个月注射一次并按需治疗),共治疗 24 个月。在接受三次诱导注射后,湿性黄斑风险影响视觉预后,该风险由光学相干断层扫描记录的初始脉络膜厚血管(黄斑最大垂直脉络膜血管直径 [CVD]≥180μm)和厚脉络膜(中央脉络膜厚度 [CCT]≥220μm)预测。无论是否存在厚脉络膜,厚血管组的复发性渗出性变化风险均更高。当达到干性黄斑时,抗 VEGF 治疗会导致平均 CVD 和 CCT 降低,这表明渗出性变化受 VEGF 调节。在缓解期时,初始厚血管和厚脉络膜患者的平均 CVD 和 CCT 高于无厚血管和厚脉络膜患者;CVD 和 CCT 的基线水平很可能代表与 VEGF 无关的条件。CVD 增加先于 CCT 增加和复发性渗出性变化,这表明与 VEGF 相关的 CVD 增加可能调节 CCT 和渗出性变化;并且 CVD 可能是渗出性变化的生物标志物。

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