病例报告:一名黑色素瘤相关视网膜病变患者的纵向评估和治疗。

Ryan Mosavi-Hecht, Paul Yang, Barrett Heyer, Christopher R Rosenberg, Elizabeth White, Elizabeth G Berry, Robert M Duvoisin, Catherine W Morgans
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引用次数: 0

摘要

黑色素瘤相关视网膜病变(MAR)是一种与皮肤转移性黑色素瘤相关的副肿瘤综合征,患者会出现视力障碍,包括夜视能力下降、对比敏感度差和光视。MAR是由针对TRPM1的自身抗体引起的,TRPM1是一种存在于黑色素细胞和视网膜ON-双极细胞(ON-BC)中的离子通道。当 TRPM1 自身抗体进入 ON-BC 并阻断 TRPM1 的功能时,就会出现视觉症状,因此检测患者血清中的 TRPM1 自身抗体是诊断 MAR 的关键标准。视网膜电图用于测量TRPM1自身抗体对ON-BC功能的影响,是MAR的另一个重要诊断工具。迄今为止,MAR 病例报告都包含其中一种或两种诊断成分,但只针对患者病程中的一个时间点。在此,我们报告了一例通过对血清自身抗体检测、视觉功能、眼部炎症、血管完整性和对缓释眼内皮质类固醇的反应进行纵向分析来支持的MAR病例。将这些数据与患者的肿瘤学和眼科记录相结合,可以发现有关MAR发病机制、进展和治疗的新见解,这些见解可以为新的研究提供信息,并扩展我们对该疾病的集体认识。简而言之,我们发现即使血清中的TRPM1自身抗体水平几乎无法通过Western印迹和免疫组化检测到,TRPM1自身抗体也会破坏视力;尽管循环中的TRPM1自身抗体水平很高,但眼内地塞米松治疗可减轻MAR的视觉症状,这表明抗体进入视网膜是MAR发病机制中的一个关键因素。患者眼睛中炎症细胞因子水平升高可能是造成所观察到的血-视网膜屏障损伤以及随后自身抗体进入视网膜的原因。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Case Report: Longitudinal Evaluation and Treatment of a Melanoma-Associated Retinopathy Patient.

Melanoma-associated retinopathy (MAR) is a paraneoplastic syndrome associated with cutaneous metastatic melanoma in which patients develop vision deficits that include reduced night vision, poor contrast sensitivity, and photopsia. MAR is caused by autoantibodies targeting TRPM1, an ion channel found in melanocytes and retinal ON-bipolar cells (ON-BCs). The visual symptoms arise when TRPM1 autoantibodies enter ON-BCs and block the function of TRPM1, thus detection of TRPM1 autoantibodies in patient serum is a key criterion in diagnosing MAR. Electroretinograms are used to measure the impact of TRPM1 autoantibodies on ON-BC function and represent another important diagnostic tool for MAR. To date, MAR case reports have included one or both diagnostic components, but only for a single time point in the course of a patient's disease. Here, we report a case of MAR supported by longitudinal analysis of serum autoantibody detection, visual function, ocular inflammation, vascular integrity, and response to slow-release intraocular corticosteroids. Integrating these data with the patient's oncological and ophthalmological records reveals novel insights regarding MAR pathogenesis, progression, and treatment, which may inform new research and expand our collective understanding of the disease. In brief, we find TRPM1 autoantibodies can disrupt vision even when serum levels are barely detectable by western blot and immunohistochemistry; intraocular dexamethasone treatment alleviates MAR visual symptoms despite high levels of circulating TRPM1 autoantibodies, implicating antibody access to the retina as a key factor in MAR pathogenesis. Elevated inflammatory cytokine levels in the patient's eyes may be responsible for the observed damage to the blood-retinal barrier and subsequent entry of autoantibodies into the retina.

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