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模拟多色离焦对眼生物测量的反应。

Ocular biometric responses to simulated polychromatic defocus.

机构信息

Herbert Wertheim School of Optometry and Vision Science, University of California, Berkeley, Berkeley, CA, USA.

Google X, Mountain View, CA, USA.

出版信息

J Vis. 2024 Nov 4;24(12):3. doi: 10.1167/jov.24.12.3.

Abstract

Evidence from human studies of ocular accommodation and studies of animals reared in monochromatic conditions suggest that chromatic signals can guide ocular growth. We hypothesized that ocular biometric response in humans can be manipulated by simulating the chromatic contrast differences associated with imposition of optical defocus. The red, green, and blue (RGB) channels of an RGB movie of the natural world were individually incorporated with computational defocus to create two different movie stimuli. The magnitude of defocus incorporated in the red and blue layers was chosen such that, in one case, it simulated +3 D defocus, referred to as color-signed myopic (CSM) defocus, and in another case it simulated -3 D defocus, referred to as color-signed hyperopic (CSH) defocus. Seventeen subjects viewed the reference stimulus (unaltered movie) and at least one of the two color-signed defocus stimuli for ∼1 hour. Axial length (AL) and choroidal thickness (ChT) were measured immediately before and after each session. AL and subfoveal ChT showed no significant change under any of the three conditions. A significant increase in vitreous chamber depth (VCD) was observed following viewing of the CSH stimulus compared with the reference stimulus (0.034 ± 0.03 mm and 0 ± 0.02 mm, respectively; p = 0.018). A significant thinning of the crystalline lens was observed following viewing of the CSH stimulus relative to the CSM stimulus (-0.033 ± 0.03 mm and 0.001 ± 0.03 mm, respectively; p = 0.015). Differences in the effects of CSM and CSH conditions on VCD and lens thickness suggest a directional, modulatory influence of chromatic defocus. On the other hand, ChT responses showed large variability, rendering it an unreliable biomarker for chromatic defocus-driven responses, at least for the conditions of this study.

摘要

来自人类眼调节研究和单色环境中饲养动物的研究证据表明,色觉信号可以引导眼球生长。我们假设,通过模拟与光学离焦相关的色觉对比度差异,可以人为操控人类眼球生物测量的反应。将自然世界的 RGB 电影的红、绿、蓝(RGB)通道分别与计算性离焦相结合,以创建两种不同的电影刺激。在红色和蓝色层中加入的离焦量选择为在一种情况下模拟+3D 离焦,称为色觉标记性近视(CSM)离焦,而在另一种情况下模拟-3D 离焦,称为色觉标记性远视(CSH)离焦。17 名受试者观看参考刺激(未改变的电影)和两种色觉标记离焦刺激中的至少一种,时间约为 1 小时。在每次测试前后立即测量眼轴(AL)和脉络膜厚度(ChT)。在任何三种情况下,AL 和中心凹下 ChT 均无明显变化。与参考刺激相比,在观看 CSH 刺激后,玻璃体腔深度(VCD)显著增加(分别为 0.034±0.03mm 和 0±0.02mm,p=0.018)。与 CSM 刺激相比,在观看 CSH 刺激后,晶状体明显变薄(分别为-0.033±0.03mm 和 0.001±0.03mm,p=0.015)。CSM 和 CSH 条件对 VCD 和晶状体厚度的影响差异表明,色觉离焦具有方向性、调节性影响。另一方面,ChT 反应的变异性很大,使其成为对色觉离焦驱动反应的不可靠生物标志物,至少对于本研究的条件是如此。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3e2f/11540029/068d6953710f/jovi-24-12-3-f001.jpg

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