Clinical and anatomical features of myopia

IF 3.7 3区 医学 Q1 OPHTHALMOLOGY
Jost B. Jonas , Songhomitra Panda-Jonas , Li Dong , Rahul A. Jonas
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Abstract

The purpose of the review is to summarize clinical and anatomically-related aspects of myopia. Recent studies have revealed macular atrophy as myopic maculopathy (MMP) stage-4 was accompanied by a central Bruch´s membrane (BM) defect associated with a subretinal proliferation (as sign of previous macular neovascularization). Patchy atrophies (MMP-stage 3) could be differentiated into those without versus with BM defects/subretinal proliferations. BM defects and subretinal proliferations were associated with each other (OR: 78.3; P < 0.001). Fundus tessellation as MMP-stage-1 correlated with visual acuity reduction, suggesting pathological changes already at MMP stage 1, in addition to a leptochoroid as risk factor. Myopic parapapillary beta zone (potentially caused by an axial elongation-related enlargement of the retinal pigment epithelium [RPE] layer opening; characterized by small or no alpha zone, few or no RPE drusen at its border, normal BM thickness) can be differentiated from glaucomatous parapapillary beta zone (characterized by alpha zone, RPE drusen, and thickened BM). The overlying retinal layers extended into the parapapillary zones, deeper than the superficial layers. Prevalence of non-glaucomatous optic neuropathy increased non-linearly with longer axial length in highly myopic eyes and was a major cause for vision loss in high myopia. In patients aged 85 + years, prevalence of MMP stage 3 or 4 in highly myopic eyes (axial length ≥ 26.5 mm) was about 75 %. Myopia was associated with a lower prevalence of diabetic retinopathy, age-related macular degeneration and angle-closure glaucoma, while high myopia, more than moderate myopia, was associated with higher prevalence and incidence of open-angle glaucoma.
近视的临床与解剖学特征。
综述的目的是总结近视的临床和解剖学相关方面。最近的研究表明,黄斑萎缩为近视黄斑病变(MMP) 4期伴有中央布鲁氏膜(BM)缺损,并伴有视网膜下增生(作为先前黄斑新生血管的标志)。斑片状萎缩(mmp - 3期)可以区分为无基底膜缺损或视网膜下增生。基底膜缺损与视网膜下增生相互关联(OR: 78.3;P < 0.001)。MMP- 1期时眼底再裂与视力下降相关,提示MMP- 1期已发生病理改变,此外细脉络膜是危险因素。近视的乳头旁β区(可能是由于视网膜色素上皮[RPE]层开口轴向伸长引起的扩大;青光眼乳头旁β带(以α带、RPE结节、BM厚度正常为特征)与α带、RPE结节、BM增厚为特征。覆盖的视网膜层延伸到乳头旁区,比浅层更深。非青光眼性视神经病变在高度近视眼中的患病率随着眼轴长度的增加呈非线性增加,是高度近视视力丧失的主要原因。在85岁以上的患者中,高度近视眼(眼轴长度≥26.5mm)的3期或4期MMP患病率约为75%。近视与糖尿病视网膜病变、年龄相关性黄斑变性和闭角型青光眼的患病率较低相关,而高度近视比中度近视与开角型青光眼的患病率和发病率较高相关。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
8.10
自引率
18.20%
发文量
197
审稿时长
6 weeks
期刊介绍: The Asia-Pacific Journal of Ophthalmology, a bimonthly, peer-reviewed online scientific publication, is an official publication of the Asia-Pacific Academy of Ophthalmology (APAO), a supranational organization which is committed to research, training, learning, publication and knowledge and skill transfers in ophthalmology and visual sciences. The Asia-Pacific Journal of Ophthalmology welcomes review articles on currently hot topics, original, previously unpublished manuscripts describing clinical investigations, clinical observations and clinically relevant laboratory investigations, as well as .perspectives containing personal viewpoints on topics with broad interests. Editorials are published by invitation only. Case reports are generally not considered. The Asia-Pacific Journal of Ophthalmology covers 16 subspecialties and is freely circulated among individual members of the APAO’s member societies, which amounts to a potential readership of over 50,000.
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