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玻璃膜疣病变:源自同一共同途径的多种病因。

Vitelliform maculopathy: Diverse etiologies originating from one common pathway.

机构信息

Eye Clinic, Multidisciplinary Department of Medical, Surgical and Dental Sciences, University of Campania Luigi Vanvitelli, Naples, Italy.

Vitreous Retina Macula Consultants of New York, New York, NY, USA.

出版信息

Surv Ophthalmol. 2023 May-Jun;68(3):361-379. doi: 10.1016/j.survophthal.2023.01.009. Epub 2023 Jan 30.

DOI:10.1016/j.survophthal.2023.01.009
PMID:36720370
Abstract

Vitelliform lesions (VLs) are associated with a wide array of macular disorders but are the result of one common pathway: retinal pigment epithelium (RPE) impairment and phagocytic dysfunction. VLs are defined by the accumulation of yellowish subretinal material. In the era of multimodal advanced retinal imaging, VLs can be further characterized by subretinal hyperreflectivity with optical coherence tomography and hyperautofluorescence with fundus autofluorescence. VLs can be the result of genetic or acquired retinal diseases. In younger patients, VLs usually occur in the setting of Best disease. Additional genetic causes of VL include pattern dystrophy or adult-onset vitelliform macular dystrophy. In older patients, acquired VLs can be associated with a broad spectrum of etiologies, including tractional, paraneoplastic, toxic, and degenerative disorders. The main cause of visual morbidity in eyes with VLs is the onset of macular atrophy and macular neovascularization. Histopathological studies have provided new insights into the location, nature, and lifecycle of the vitelliform material comprised of melanosomes, lipofuscin, melanolipofuscin, and outer segment debris located between the RPE and photoreceptor layer. Impaired phagocytosis by the RPE cells is the unifying pathway leading to VL development. We discuss and summarize the nature, pathogenesis, multimodal imaging characteristics, etiologies, and natural course of vitelliform maculopathies.

摘要

玻璃膜疣(VLs)与广泛的黄斑疾病有关,但它们是由一个共同的途径引起的:视网膜色素上皮(RPE)损伤和吞噬功能障碍。VLs 的定义是黄色的视网膜下物质的积累。在多模态高级视网膜成像的时代,VLs 可以通过视网膜下高反射性与光学相干断层扫描和眼底自发荧光的高自发荧光来进一步描述。VLs 可以是遗传或获得性视网膜疾病的结果。在年轻患者中,VLs 通常发生在 Best 病的背景下。VLs 的其他遗传原因包括模式营养不良或成人型卵黄样黄斑营养不良。在老年患者中,获得性 VLs 可与广泛的病因相关,包括牵引性、副肿瘤性、毒性和退行性疾病。VLs 眼中视力受损的主要原因是黄斑萎缩和黄斑新生血管的发生。组织病理学研究为位于 RPE 和光感受器层之间的由黑素体、脂褐素、黑素脂褐素和外节碎片组成的卵黄样物质的位置、性质和生命周期提供了新的见解。RPE 细胞的吞噬功能受损是导致 VL 发展的统一途径。我们讨论并总结了卵黄样黄斑病变的性质、发病机制、多模态成像特征、病因和自然病程。

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