Labrique Alain B, Palmer Amanda C, Healy Katherine, Mehra Sucheta, Sauer Theodor C, West Keith P, Sommer Alfred
Department of International Health, Johns Hopkins Bloomberg School of Public Health, Baltimore, MD, USA.
BMC Ophthalmol. 2015 Jul 9;15:74. doi: 10.1186/s12886-015-0062-7.
Aberrant dark adaptation is common to many ocular diseases and pathophysiological conditions, including vitamin A deficiency, cardiopulmonary diseases, and hypoxia. Scotopic vision and pupillary responsiveness have typically been measured using subjective, time-consuming methods. Existing techniques are particularly challenging for use in developing country settings, where vitamin A deficiency remains a major public health problem. Our aim was design a compact, low cost, and easily operated device to assess dark adaptation in the field.
The Portable Field Dark Adaptometer (PFDA) incorporates a digital camera, a retinal bleaching flash, and a Ganzfeld light source inside a pair of light-obscuring goggles. After a ~10 min period of dark adaption, the infrared camera digitally records afferent pupillary responses to graded light stimuli (-2.9 to 0.1 log cd/m(2)). We tested this device in a variety of field settings to assess: a) ease of use and b) whether test data could clearly and accurately depict the well-known dose-response relationship between light intensity and pupil contraction. A total of 822 videos were collected. We used an open source video analysis software to measure pupil size in pixel units. Pupillary responsiveness was expressed as the percent change in pupil size from pre- to post-light exposure. Box plots, t test, and multi-level mixed effects linear regression modeling were used to characterize the relationship between light intensity and pupillary response.
The PFDA was employed with only minor technical challenges in Bangladesh, Kenya, Zambia, and Peru. Our data show a clear linear increase in pupillary constriction with increasing log light intensity. Light intensity was a strong predictor of pupillary response, regardless of baseline pupil size.
The consistent physiological response demonstrated here supports the use of the PFDA as a reliable tool to measure dark adaptation. As a next step, PFDA measurements will be validated against biochemical indicators of vitamin A status and hypoxemia. Ultimately, this new technology may provide a novel approach for nutritional assessment, with potential clinical applications.
异常暗适应在许多眼部疾病和病理生理状况中很常见,包括维生素A缺乏症、心肺疾病和缺氧。暗视觉和瞳孔反应性通常使用主观、耗时的方法进行测量。现有技术在发展中国家环境中使用尤其具有挑战性,因为维生素A缺乏仍然是一个主要的公共卫生问题。我们的目标是设计一种紧凑、低成本且易于操作的设备,用于在现场评估暗适应。
便携式现场暗适应计(PFDA)在一副遮光护目镜内集成了一台数码相机、一次视网膜漂白闪光和一个全视野光源。经过约10分钟的暗适应期后,红外相机以数字方式记录对分级光刺激(-2.9至0.1 log cd/m²)的传入瞳孔反应。我们在各种现场环境中对该设备进行了测试,以评估:a)易用性;b)测试数据是否能够清晰、准确地描绘光强度与瞳孔收缩之间众所周知的剂量反应关系。总共收集了822个视频。我们使用开源视频分析软件以像素单位测量瞳孔大小。瞳孔反应性表示为光照前后瞳孔大小的变化百分比。使用箱线图、t检验和多级混合效应线性回归模型来表征光强度与瞳孔反应之间的关系。
在孟加拉国、肯尼亚、赞比亚和秘鲁,PFDA的使用仅面临一些小的技术挑战。我们的数据显示,随着对数光强度的增加,瞳孔收缩呈明显的线性增加。无论基线瞳孔大小如何,光强度都是瞳孔反应的有力预测指标。
此处展示的一致生理反应支持将PFDA用作测量暗适应的可靠工具。下一步,将根据维生素A状态和低氧血症的生化指标对PFDA测量结果进行验证。最终,这项新技术可能为营养评估提供一种新方法,并具有潜在的临床应用价值。
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