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特发性脉络膜新生血管患者黄斑区视网膜内层选择性变薄:羟氯喹视网膜毒性的早期征象

Selective thinning of the perifoveal inner retina as an early sign of hydroxychloroquine retinal toxicity.

机构信息

Department of Ophthalmology and Visual Sciences, Eye and Ear Infirmary, University of Illinois at Chicago, Chicago, IL 60612, USA.

出版信息

Eye (Lond). 2010 May;24(5):756-62; quiz 763. doi: 10.1038/eye.2010.21. Epub 2010 Apr 16.

Abstract

PURPOSE

To evaluate macular thickness profiles using spectral-domain optical coherence tomography (SDOCT) and image segmentation in patients with chronic exposure to hydroxychloroquine.

METHODS

This study included eight patients with chronic exposure to hydroxychloroquine (group 1) and eight controls (group 2). Group 1 patients had no clinically evident retinal toxicity. All subjects underwent SDOCT imaging of the macula. An image segmentation technique was used to measure thickness of six retinal layers at 200 microm intervals. A mixed-effects model was used for multivariate analysis.

RESULTS

By measuring total retinal thickness either at the central macular (2800 microm in diameter), the perifoveal region 1200-microm-width ring surrounding the central macula), or the overall macular area (5200 microm in diameter), there were no significant differences in the thickness between groups 1 and 2. On an image segmentation analysis, selective thinning of the inner plexiform+ganglion cell layers (P=0.021) was observed only in the perifoveal area of the patients in group 1 compared with that of group 2 by using the mixed-effects model analysis.

CONCLUSION

Our study results suggest that chronic exposure to hydroxychloroquine is associated with thinning of the perifoveal inner retinal layers, especially in the ganglion cell and inner plexiform layers, even in the absence of functional or structural clinical changes involving the photoreceptor or retinal pigment epithelial cell layers. This may be a contributing factor as the reason most patients who have early detectable signs of drug toxicity present with paracentral or pericentral scotomas.

摘要

目的

使用频域光相干断层扫描(SDOCT)和图像分割评估长期接受羟氯喹治疗的患者的黄斑厚度谱。

方法

本研究纳入了 8 名长期接受羟氯喹治疗的患者(1 组)和 8 名对照者(2 组)。1 组患者无明显临床视网膜毒性。所有受试者均行黄斑 SDOCT 成像。采用图像分割技术测量 200μm 间隔的 6 层视网膜厚度。采用混合效应模型进行多变量分析。

结果

通过测量中央黄斑(直径 2800μm)、中央黄斑周围 1200μm 宽的旁中心区环(peri-foveal region)和整个黄斑区(直径 5200μm)的总视网膜厚度,1 组和 2 组之间的厚度无显著差异。通过图像分割分析,仅在 1 组患者的旁中心区观察到内丛状+节细胞层的选择性变薄(P=0.021),而混合效应模型分析显示,2 组无此变化。

结论

本研究结果表明,长期接受羟氯喹治疗与旁中心区内层视网膜变薄有关,特别是在神经节细胞和内丛状层,即使在外层视网膜感光细胞和视网膜色素上皮细胞层没有功能或结构的临床改变。这可能是大多数早期发现药物毒性的患者出现中心旁或旁中心暗点的原因之一。

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