长期接受羟氯喹治疗的临床无症状系统性红斑狼疮患者视觉运动障碍的眼部生物标志物

Andrew R. Berneshawi, Kimia Seyedmadani, Rahul Goel, Mark R. Anderson, Terence L. Tyson, Yasmin M. Akay, Metin Akay, Loh-Shan B. Leung, Leland S. Stone
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摘要

本研究将一组眼球运动测量指标或 "眼球测量 "生物标志物作为无症状、长期接受羟氯喹(HCQ)治疗的系统性红斑狼疮(SLE)患者视网膜毒性引起的视觉和视觉运动障碍的潜在早期指标。我们使用以前建立的行为任务和分析技术,测量了一批长期接受 HCQ 治疗的系统性红斑狼疮患者的眼球运动反应。我们还使用双变量皮尔逊相关性和线性混合效应模型(LMM)研究了患者群体中的眼球测量、视网膜厚度的 OCT 测量和视觉功能的标准临床近视测量之间的关系。与 17 名年龄匹配的健康对照组相比,12 名长期接受 HCQ 治疗的无症状系统性红斑狼疮患者出现了明显的视觉和视觉运动障碍。值得注意的是,有六项视力测量指标存在显著差异。初始追视加速度中位数为22%,稳态追视增益中位数为16%,平滑比例中位数为7%,目标速度反应性中位数为31%,而追视囊泡振幅中位数为46%,固定误差中位数为46%。除去两名确诊为轻度中毒的患者,与对照组相比,除定点误差和平稳比例外,其他四项视力测量指标仍然存在明显缺陷。在我们的 12 名患者(24 个视网膜)中,我们发现追视延迟、初始加速度、稳态增益和固定误差与视网膜厚度呈线性关系,即使考虑到年龄因素也是如此,而临床功能的标准测量(平均偏差和模式标准偏差)则不然。我们的数据表明,特定的眼球测量法是服用HCQ的系统性红斑狼疮患者功能障碍的敏感早期生物标志物,可用于协助早期检测HCQ引起的视网膜毒性和其他视觉病变,其早期诊断价值可能超过标准视野和OCT评估。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Oculometric biomarkers of visuomotor deficits in clinically asymptomatic patients with systemic lupus erythematosus undergoing long-term hydroxychloroquine treatment
This study examines a set of oculomotor measurements, or “oculometric” biomarkers, as potential early indicators of visual and visuomotor deficits due to retinal toxicity in asymptomatic Systemic Lupus Erythematosus (SLE) patients on long-term hydroxychloroquine (HCQ) treatment. The aim is to identify subclinical functional impairments that are otherwise undetectable by standard clinical tests and to link them to structural retinal changes.We measured oculomotor responses in a cohort of SLE patients on chronic HCQ therapy using a previously established behavioral task and analysis technique. We also examined the relationship between oculometrics, OCT measures of retinal thickness, and standard clinical perimetry measures of visual function in our patient group using Bivariate Pearson Correlation and a Linear Mixed-Effects Model (LMM).Significant visual and visuomotor deficits were found in 12 asymptomatic SLE patients on long-term HCQ therapy compared to a cohort of 17 age-matched healthy controls. Notably, six oculometrics were significantly different. The median initial pursuit acceleration was 22%, steady-state pursuit gain 16%, proportion smooth 7%, and target speed responsiveness 31% lower, while catch-up saccade amplitude was 46% and fixation error 46% larger. Excluding the two patients with diagnosed mild toxicity, four oculometrics, all but fixation error and proportion smooth, remained significantly impaired compared to controls. Across our population of 12 patients (24 retinae), we found that pursuit latency, initial acceleration, steady-state gain, and fixation error were linearly related to retinal thickness even when age was accounted for, while standard measures of clinical function (Mean Deviation and Pattern Standard Deviation) were not.Our data show that specific oculometrics are sensitive early biomarkers of functional deficits in SLE patients on HCQ that could be harnessed to assist in the early detection of HCQ-induced retinal toxicity and other visual pathologies, potentially providing early diagnostic value beyond standard visual field and OCT evaluations.
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