Singapore Eye Research Institute, Singapore National Eye Centre, 11 Third Hospital Avenue, Singapore, 168751, Singapore.
Duke-NUS Medical School, National University of Singapore, Singapore, Singapore.
Sci Rep. 2022 Feb 22;12(1):2993. doi: 10.1038/s41598-022-06742-2.
The aim of this study was to evaluate influence of baseline imaging features on visual and anatomical outcomes in eyes with PCV treated with anti-VEGF monotherapy. In this prospective study we enrolled participants with treatment-naïve PCV who followed a treat-and-extend protocol using intravitreal aflibercept (IVA) monotherapy. Baseline clinical features evaluatedincluded best corrected visual acuity (BCVA), traditional features such as lesion size, fluid-related OCT parameters and novel parameters using automated software. This included quantitative and qualitative pigment epithelium detachment (PED) parameters [height, volume]; and choroidal parameters. [choroidal thickness (CT), choroidal volume (CV) and choroidal vascularity index (CVI). We evaluated the predictive value of each parameter on visual and anatomical outcome at month 12. We additionally evaluated initial treatment response after 3 monthly injections with respect to month 12 outcomes. Fifty-two eyes from 52 participants were included in the study. The BCVA increased from 61.1 ± 13.2 to 69.6 ± 13.2 early treatment diabetic retinopathy study (ETDRS) letters (p < 0.01) and CRT reduced from 455.7 ± 182.4 µm to 272.7 ± 86.2 (p < 0.01) from baseline to month 12. The proportion of eyes with PED decreased significant from 100% at baseline to 80% at month 12 (p < 0.01). Reduction in the mean maximum height of PED (from 381.3 ± 236.3 µm to 206.8 vs ± 146.4 µm) and PED volume (from 1322 ± 853 nl to 686 ± 593 nl) (p < 0.01) was also noted from baseline to month12. Baseline features associated with better month 12 BCVA included baseline BCVA (β = - 0.98, 95%CI - 3.38 to - 1.61, p = 0.02) and baseline CRT (β = - 0.98, 95%CI - 1.56 to - 0.40, p = 0.04) while the disease activity at month12 was significantly associated with lower baseline CRT (366.0 ± 129.5 vs 612.0 ± 188.0 , p < 0.001), lower baseline PED height (242.0 ± 150.0 vs 542.0 ± 298.0 µm, p < 0.01), lower baseline PED volume (0.6 ± 0.3 mm vs 2.2 ± 1.3 mm vs, p < 0.01), lower proportion with marked CVH (17.9% vs 46.2%, p = 0.02) and lower mean CVI (61.8 ± 1.4 vs 63.0 ± 1.4, p < 0.02). Additionally, a larger decrease in CRT (per 100 nm) and larger PED volume reduction (per 100 nl) at month 3 from baseline were associated with greater BCVA gain and inactive disease. PED-related volumetric parameters have an additional predictive value to traditional biomarkers of disease activity in eyes with PCV undergoing anti-VEGF monotherapy. With increasingly precise quantification, PEDs can be a crucial biomarker in addition to traditional parameters and may aid in retreatment decisions.
本研究旨在评估基线影像学特征对接受抗 VEGF 单药治疗的 PCV 眼视觉和解剖结果的影响。在这项前瞻性研究中,我们纳入了接受治疗-naive PCV 并遵循玻璃体内阿柏西普(IVA)单药治疗的延长治疗方案的患者。基线临床特征评估包括最佳矫正视力(BCVA)、传统特征(如病变大小)、液体相关的 OCT 参数以及使用自动软件的新型参数。这包括定量和定性的色素上皮脱离(PED)参数[高度、体积];和脉络膜参数。[脉络膜厚度(CT)、脉络膜体积(CV)和脉络膜血管指数(CVI)。我们评估了每个参数在第 12 个月时的视觉和解剖结果的预测价值。我们还评估了第 3 个月治疗后的初始治疗反应与第 12 个月的结果。共有 52 名患者的 52 只眼纳入研究。BCVA 从 61.1±13.2 个早期治疗糖尿病视网膜病变研究(ETDRS)字母增加到 69.6±13.2 个字母(p<0.01),CRT 从基线时的 455.7±182.4µm 减少到 272.7±86.2µm(p<0.01)。基线时 PED 的比例从 100%下降到 12 个月时的 80%(p<0.01)。从基线到第 12 个月,PED 的平均最大高度(从 381.3±236.3µm 降至 206.8±146.4µm)和 PED 体积(从 1322±853nl 降至 686±593nl)(p<0.01)也有所下降。与第 12 个月 BCVA 较好相关的基线特征包括基线 BCVA(β=-0.98,95%CI-3.38 至-1.61,p=0.02)和基线 CRT(β=-0.98,95%CI-1.56 至-0.40,p=0.04),而第 12 个月的疾病活动度与较低的基线 CRT 显著相关(366.0±129.5 与 612.0±188.0,p<0.001),较低的基线 PED 高度(242.0±150.0 与 542.0±298.0µm,p<0.01),较低的基线 PED 体积(0.6±0.3mm 与 2.2±1.3mm,p<0.01),较低的标记 CVH 比例(17.9%与 46.2%,p=0.02)和较低的平均 CVI(61.8±1.4 与 63.0±1.4,p<0.02)。此外,第 3 个月时 CRT (每 100nm)和 PED 体积(每 100nl)的较大减少与 BCVA 的较大增加和疾病的不活跃相关。在接受抗 VEGF 单药治疗的 PCV 眼中,PED 相关的容积参数对疾病活动的传统生物标志物具有额外的预测价值。随着定量的不断精确,PED 除了传统参数外还可以成为一个重要的生物标志物,并可能有助于再治疗决策。
