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在接受1年固定剂量阿柏西普治疗后达到非活动性息肉样脉络膜血管病变后出现复发性息肉样病变。

Recurrent polypoidal lesions after achieving inactive polypoidal choroidal vasculopathy following 1-year fixed-dosing aflibercept treatments.

作者信息

Chaikitmongkol Voraporn, Tadadoltip Wantip, Patikulsila Direk, Srisomboon Titipol, Narongchai Chanusnun, Choovuthayakorn Janejit, Watanachai Nawat, Kunavisarut Paradee, Sangkaew Apisara, Upaphong Phit, Bressler Neil M

机构信息

Retina Division, Department of Ophthalmology, Faculty of Medicine, Chiang Mai University, Chiang Mai, Thailand.

Department of Ophthalmology, Faculty of Medicine, Chiang Mai University, Chiang Mai, Thailand.

出版信息

Asia Pac J Ophthalmol (Phila). 2025 Mar-Apr;14(2):100176. doi: 10.1016/j.apjo.2025.100176. Epub 2025 Mar 1.

Abstract

PURPOSE

Polypoidal choroidal vasculopathy (PCV) may have frequent recurrences after fluid resolution, but time to recurrence is unclear. This study explored time to first polypoidal recurrence after 1-year fixed-dosing aflibercept treatments.

DESIGN

Retrospective cohort study.

METHODS

Treatment-naïve PCV eyes treated between April 2015 to May 2019 were identified and included with criteria including: (1) received fixed-dosing 2 mg aflibercept in the first year, (2) became "inactive" (absence of both intraretinal and subretinal fluid on OCT) at post-treatment year-1 (PTY1) and managed as needed (PRN) thereafter, (3) FU ≥ 12 months after PTY1. Fundus photography, indocyanine green angiography (ICGA), and OCT graded to identify timing and risk factors for recurrence (defined as fluid on OCT).

RESULTS

Of 37 study eyes [37 patients; median age was 64 years (IQR 59-69); median aflibercept injection number was 8 (IQR 8-8); median FU 38 months (IQR, 30-50 months)]; 18 eyes (49 %) had recurrence during FU. Fourteen (78 %) of 18 had recurrence within 12 months after PTY1 visit. Risk factors for recurrence included: incomplete polypoidal regression on post-treatment ICGA [P = .004, Hazard ratio (HR) = 4.4, 95 % confidence interval (CI) 1.6-11.9] and PED with internal heterogeneous reflectivity on post-treatment OCT (P = .04, HR = 2.7, 95 % CI 1.1-6.9).

CONCLUSIONS

Nearly half of inactive PCV eyes following 1-year fixed-dosing aflibercept treatments had recurrent polypoidal lesions. Eyes with high-risk features for recurrence, some of which can be detected with OCT without the need for ICGA, may warrant close monitoring.

摘要

目的

息肉样脉络膜血管病变(PCV)在积液消退后可能频繁复发,但复发时间尚不清楚。本研究探讨了在接受1年固定剂量阿柏西普治疗后首次息肉样复发的时间。

设计

回顾性队列研究。

方法

确定并纳入2015年4月至2019年5月间初治的PCV患眼,纳入标准包括:(1)第一年接受2mg阿柏西普固定剂量治疗;(2)在治疗后第1年(PTY1)时变为“静止”(OCT检查无视网膜内和视网膜下液),此后按需治疗(PRN);(3)PTY1后随访≥12个月。通过眼底照相、吲哚菁绿血管造影(ICGA)和OCT分级来确定复发的时间和危险因素(定义为OCT上出现积液)。

结果

37只研究患眼[37例患者;中位年龄64岁(四分位间距59 - 69岁);阿柏西普注射次数中位数为8次(四分位间距8 - 8次);中位随访38个月(四分位间距,30 - 50个月)];18只眼(49%)在随访期间复发。18只眼中有14只(78%)在PTY1就诊后12个月内复发。复发的危险因素包括:治疗后ICGA上息肉样病变消退不完全[P = 0.0),危险比(HR)= 4.4,95%置信区间(CI)1.6 - 11.9]和治疗后OCT上具有内部异质性反射率的PED(P = 0.04,HR = 6.9)。

结论

在接受1年固定剂量阿柏西普治疗后,近一半静止的PCV患眼出现息肉样病变复发。具有复发高危特征的患眼,其中一些可通过OCT检测而无需ICGA,可能需要密切监测。

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