International Photographic Classification and Grading System for Myopic Maculopathy

黄斑病 医学 眼科 科恩卡帕 验光服务 分级(工程) 眼底(子宫) 眼底摄影 视网膜 视网膜病变 荧光血管造影 计算机科学 糖尿病 内分泌学 机器学习 土木工程 工程类
作者
Kyoko Ohno‐Matsui,Ryo Kawasaki,Jost B. Jonas,Chui Ming Gemmy Cheung,Seang‐Mei Saw,Virginie J. M. Verhoeven,Caroline C. W. Klaver,Muka Moriyama,Kosei Shinohara,Yumiko Kawasaki,Mai Yamazaki,Stacy M. Meuer,Tatsuro Ishibashi,Miho Yasuda,Hidetoshi Yamashita,Akira Sugano,Jie Jin Wang,Paul Mitchell,Tien Yin Wong,Kyoko Ohno‐Matsui,Muka Moriyama,Kosei Shinohara,Ryo Kawasaki,Yumiko Kawasaki,Mai Yamazaki,Jost B. Jonas,Chui-Ming Gemmy Cheung,Seang‐Mei Saw,Tien Yin Wong,Virginie J. M. Verhoeven,Caroline C. W. Klaver,Stacy M. Meuer,Ronald Klein,Ronald Klein,Tatsuro Ishibashi,Miho Yasuda,Akira Sugano,Hidetoshi Yamashita,Jie Jin Wang,Paul Mitchell,Ning Li Wang,Hassan Hashemi,Akbar Fotouhi,Ozren Polašek,Véronique Vitart,James F. Wilson,Brian W. Fleck
出处
期刊:American Journal of Ophthalmology [Elsevier]
卷期号:159 (5): 877-883.e7 被引量:625
标识
DOI:10.1016/j.ajo.2015.01.022
摘要

Purpose To develop a classification and grading system for myopic maculopathy. Design Development and evaluation of a classification system for myopic maculopathy based on observational case series. Methods A comprehensive set of myopic macular lesions was defined via literature review and through consensus meetings among retinal specialists and clinician scientists. A classification of myopic maculopathy was formulated based on fundus photographs and a modified Delphi process and consensus. Inter- and intraobserver reproducibility, assessed as agreement (%) and weighted kappa values, were evaluated. One hundred retinal photographs with myopia and myopic macular lesions were selected from case series at the High Myopia Clinic of the Tokyo Medical and Dental University, Tokyo, Japan. Results We defined 5 categories of myopic maculopathy including “no myopic retinal degenerative lesion” (Category 0), “tessellated fundus” (Category 1), “diffuse chorioretinal atrophy” (Category 2), “patchy chorioretinal atrophy” (Category 3), and “macular atrophy” (Category 4). Three additional features to supplement these categories were defined as “plus” lesions, namely, lacquer cracks, myopic choroidal neovascularization, and Fuchs spot. Posterior staphyloma was considered as a further, important sign of myopic retinopathy. The intraobserver agreement was ≥85% and the corresponding weighted kappa statistic was ≥0.6 between observations. After a brief training session, interobserver kappa statistics reached the predefined satisfactory level (≥0.4), considered as above moderate agreement. Conclusions We propose a classification system for myopic maculopathy that was found to be reproducible. Applying a uniform classification in different studies will facilitate communication and comparison of findings from clinical trials and epidemiologic studies. To develop a classification and grading system for myopic maculopathy. Development and evaluation of a classification system for myopic maculopathy based on observational case series. A comprehensive set of myopic macular lesions was defined via literature review and through consensus meetings among retinal specialists and clinician scientists. A classification of myopic maculopathy was formulated based on fundus photographs and a modified Delphi process and consensus. Inter- and intraobserver reproducibility, assessed as agreement (%) and weighted kappa values, were evaluated. One hundred retinal photographs with myopia and myopic macular lesions were selected from case series at the High Myopia Clinic of the Tokyo Medical and Dental University, Tokyo, Japan. We defined 5 categories of myopic maculopathy including “no myopic retinal degenerative lesion” (Category 0), “tessellated fundus” (Category 1), “diffuse chorioretinal atrophy” (Category 2), “patchy chorioretinal atrophy” (Category 3), and “macular atrophy” (Category 4). Three additional features to supplement these categories were defined as “plus” lesions, namely, lacquer cracks, myopic choroidal neovascularization, and Fuchs spot. Posterior staphyloma was considered as a further, important sign of myopic retinopathy. The intraobserver agreement was ≥85% and the corresponding weighted kappa statistic was ≥0.6 between observations. After a brief training session, interobserver kappa statistics reached the predefined satisfactory level (≥0.4), considered as above moderate agreement. We propose a classification system for myopic maculopathy that was found to be reproducible. Applying a uniform classification in different studies will facilitate communication and comparison of findings from clinical trials and epidemiologic studies.
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