Interreader and Intermodality Variability in Macular Atrophy Quantification in Neovascular Age-related Macular Degeneration: Comparison of 6 Imaging Modalities.

IF 4.4 Q1 OPHTHALMOLOGY Ophthalmology. Retina Pub Date : 2024-08-30 DOI:10.1016/j.oret.2024.08.017

Enrico Borrelli, Chiara Olivieri, Sonia Serafino, Andrea Coletto, Federico Ricardi, Giovanni Neri, Paola Marolo, Michele Reibaldi

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Abstract

Purpose: Macular atrophy is a common complication in neovascular age-related macular degeneration (AMD) and is associated with poorer visual outcomes. This study evaluated interreader and intermodality variability in measuring macular atrophy in previously treated neovascular AMD eyes without exudation using 6 imaging modalities.

Design: Prospective, cohort study.

Participants: Thirty participants with previously treated neovascular AMD showing no signs of exudation at the time of enrollment and exhibiting macular atrophy.

Methods: During the same clinic visit, patients were imaged using 6 different imaging modalities: color fundus photography (CFP; Clarus, Carl Zeiss Meditec), near-infrared imaging (NIR; Spectralis, Heidelberg Engineering), structural OCT (Spectralis, Heidelberg Engineering), green fundus autofluorescence (GAF; Clarus, Carl Zeiss Meditec), blue fundus autofluorescence (BAF; Spectralis, Heidelberg Engineering), and pseudocolor imaging (MultiColor; Spectralis, Heidelberg Engineering). Two readers independently measured the macular atrophy area.

Main outcome measures: Interreader and intermodality agreement.

Results: The 95% coefficient of repeatability was 5.98 mm² for CFP, 4.46 mm² for MultiColor, 3.90 mm² for BAF, 3.92 mm² for GAF, 4.86 mm² for NIR, and 3.55 mm² for OCT. Similarly, the coefficient of variation was lowest for OCT-based grading at 0.08 and highest for NIR-based grading at 0.28. Accordingly, the intraclass correlation coefficient was 0.742 for CFP, 0.805 for MultiColor, 0.857 for BAF, 0.850 for GAF, 0.755 for NIR, and 0.917 for OCT. The 6 different imaging modalities presented measurements with different mean values, with only a limited number of comparisons not significantly different between the instruments, although measurements were correlated. The largest size of macular atrophy was measured with structural OCT-based grading (median = 4.65 mm²; interquartile range [IQR] = 4.78 mm²) and the smallest was with CFP-based grading (median = 3.86 mm²; IQR = 5.06 mm²). Inconsistencies arose from various factors.

Conclusions: In patients with neovascular AMD, macular atrophy measurements vary significantly depending on the imaging technique used. Color fundus photography-based assessments yielded the smallest macular atrophy sizes, whereas structural OCT-based assessments produced the largest. These discrepancies stem from both the inherent limitations of each modality in assessing retinal pigment epithelial atrophy and factors related to neovascularization, such as the coexistence of fibrosis.

Financial disclosure(s): Proprietary or commercial disclosure may be found in the Footnotes and Disclosures at the end of this article.

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新生血管性黄斑病变黄斑萎缩定量的阅读器间和成像模式间变异性：六种成像模式的比较。

目的：黄斑萎缩是新生血管性老年黄斑变性（AMD）的常见并发症，与较差的视觉效果有关。本研究采用六种成像模式，评估了阅片师之间和成像模式之间在测量先前治疗过的无渗出新生血管性黄斑变性眼底黄斑萎缩方面的差异：设计：前瞻性队列研究：方法：在同一门诊就诊期间，对患者进行黄斑萎缩测量：在同一次门诊中，患者使用六种不同的成像模式进行成像：彩色眼底照相（CFP；Clarus，卡尔蔡司医疗公司）、近红外成像（NIR；Spectralis；海德堡工程公司，德国海德堡）、结构性光学相干断层扫描（OCT；Spectralis；海德堡工程公司，德国海德堡）、绿色眼底自动荧光（GAF；德国海德堡海德堡工程公司）、绿色眼底自动荧光（GAF；卡尔蔡司医疗公司 Clarus）、蓝色眼底自动荧光（BAF；德国海德堡海德堡工程公司 Spectralis）和伪彩色成像（MultiColor；德国海德堡海德堡工程公司 Spectralis）。两名阅读者独立测量黄斑萎缩面积：结果：结果：CFP 的 95% 重复性系数 (CR) 为 5.98 mm2，MultiColor 为 4.46 mm2，BAF 为 3.90 mm2，GAF 为 3.92 mm2，NIR 为 4.86 mm2，OCT 为 3.55 mm2。同样，基于 OCT 分级的变异系数（CV）最低，为 0.08，而基于近红外分级的变异系数（CV）最高，为 0.28。因此，CFP 的类内相关系数（ICC）为 0.742，MultiColor 为 0.805，BAF 为 0.857，GAF 为 0.850，NIR 为 0.755，OCT 为 0.917。6 种不同成像模式的测量结果具有不同的平均值，尽管测量结果具有相关性，但只有少数仪器之间的比较结果没有显著差异。黄斑萎缩面积最大的是基于结构性OCT分级（中位数=4.65平方毫米；四分位间差[IQR]=4.78平方毫米），最小的是基于CFP分级（中位数=3.86平方毫米；IQR=5.06平方毫米）。不一致的原因是多方面的：结论：在新生血管性黄斑变性患者中，黄斑萎缩的测量值因使用的成像技术不同而存在显著差异。基于CFP的评估得出的黄斑萎缩度最小，而基于结构性OCT的评估得出的黄斑萎缩度最大。这些差异既源于每种模式在评估RPE萎缩时固有的局限性，也源于与新生血管相关的因素，如纤维化的同时存在。

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