Department of Ophthalmology, Glostrup Hospital, Ndr. Ringvej 57, 2600 Glostrup, Copenhagen, Denmark.
BMC Ophthalmol. 2012 Apr 3;12:4. doi: 10.1186/1471-2415-12-4.
The activity of melanopsin containing intrinsically photosensitive ganglion retinal cells (ipRGC) can be assessed by a means of pupil responses to bright blue (appr.480 nm) light. Due to age related factors in the eye, particularly, structural changes of the lens, less light reaches retina. The aim of this study was to examine how age and in vivo measured lens transmission of blue light might affect pupil light responses, in particular, mediated by the ipRGC.
Consensual pupil responses were explored in 44 healthy subjects aged between 26 and 68 years. A pupil response was recorded to a continuous 20 s light stimulus of 660 nm (red) or 470 nm (blue) both at 300 cd/m2 intensity (14.9 and 14.8 log photons/cm2/s, respectively). Additional recordings were performed using four 470 nm stimulus intensities of 3, 30, 100 and 300 cd/m2. The baseline pupil size was measured in darkness and results were adjusted for the baseline pupil and gender. The main outcome parameters were maximal and sustained pupil contraction amplitudes and the postillumination response assessed as area under the curve (AUC) over two time-windows: early (0-10 s after light termination) and late (10-30 s after light termination). Lens transmission was measured with an ocular fluorometer.
The sustained pupil contraction and the early poststimulus AUC correlated positively with age (p=0.02, p=0.0014, respectively) for the blue light stimulus condition only.The maximal pupil contraction amplitude did not correlate to age either for bright blue or red light stimulus conditions.Lens transmission decreased linearly with age (p<0.0001). The pupil response was stable or increased with decreasing transmission, though only significantly for the early poststimulus AUC to 300 cd/m2 light (p=0.02).
Age did not reduce, but rather enhance pupil responses mediated by ipRGC. The age related decrease of blue light transmission led to similar results, however, the effect of age was greater on these pupil responses than that of the lens transmission. Thus there must be other age related factors such as lens scatter and/or adaptive processes influencing the ipRGC mediated pupil response enhancement observed with advancing age.
通过测量瞳孔对明亮蓝光(约 480nm)的反应,可以评估含有黑视素的视网膜神经节细胞(ipRGC)的活性。由于眼睛的年龄相关因素,特别是晶状体的结构变化,较少的光到达视网膜。本研究的目的是探讨年龄和体内测量的蓝光晶状体透过率如何影响瞳孔光反应,特别是由 ipRGC 介导的光反应。
在 44 名年龄在 26 岁至 68 岁之间的健康受试者中,探索了共有的瞳孔反应。使用连续 20s 的 660nm(红光)或 470nm(蓝光)光刺激,强度均为 300cd/m2(分别为 14.9 和 14.8log 光子/cm2/s),记录瞳孔反应。使用 470nm 四种刺激强度(3、30、100 和 300cd/m2)进行了额外的记录。在黑暗中测量了基础瞳孔大小,并根据基础瞳孔和性别对结果进行了调整。主要的观察指标是最大和持续的瞳孔收缩幅度以及光照结束后 0-10s(早期)和 10-30s(晚期)的瞳孔反应面积(AUC)。使用眼荧光计测量晶状体透过率。
只有在蓝光刺激条件下,持续的瞳孔收缩和早期光后 AUC 与年龄呈正相关(p=0.02,p=0.0014)。最大瞳孔收缩幅度与年龄也无关,无论是蓝光还是红光刺激条件。晶状体透过率随年龄呈线性下降(p<0.0001)。尽管只有在 300cd/m2 光的早期光后 AUC 上差异有统计学意义(p=0.02),但随着透过率的降低,瞳孔反应是稳定的或增加的。
年龄并没有降低,而是增强了由 ipRGC 介导的瞳孔反应。与年龄相关的蓝光透过率下降导致了类似的结果,但年龄对这些瞳孔反应的影响大于对晶状体透过率的影响。因此,除了年龄相关的因素如晶状体散射和/或适应过程外,还有其他因素影响着随着年龄的增长而观察到的 ipRGC 介导的瞳孔反应增强。