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光刺激的正负反馈对基因表达的影响揭示了视觉引导眼球生长的双向机制。

Gene expression in response to optical defocus of opposite signs reveals bidirectional mechanism of visually guided eye growth.

机构信息

Department of Ophthalmology, Columbia University, New York, New York, United States of America.

College of Optometry, State University of New York, New York, New York, United States of America.

出版信息

PLoS Biol. 2018 Oct 9;16(10):e2006021. doi: 10.1371/journal.pbio.2006021. eCollection 2018 Oct.

Abstract

Myopia (nearsightedness) is the most common eye disorder, which is rapidly becoming one of the leading causes of vision loss in several parts of the world because of a recent sharp increase in prevalence. Nearwork, which produces hyperopic optical defocus on the retina, has been implicated as one of the environmental risk factors causing myopia in humans. Experimental studies have shown that hyperopic defocus imposed by negative power lenses placed in front of the eye accelerates eye growth and causes myopia, whereas myopic defocus imposed by positive lenses slows eye growth and produces a compensatory hyperopic shift in refractive state. The balance between these two optical signals is thought to regulate refractive eye development; however, the ability of the retina to recognize the sign of optical defocus and the composition of molecular signaling pathways guiding emmetropization are the subjects of intense investigation and debate. We found that the retina can readily distinguish between imposed myopic and hyperopic defocus, and identified key signaling pathways underlying retinal response to the defocus of different signs. Comparison of retinal transcriptomes in common marmosets exposed to either myopic or hyperopic defocus for 10 days or 5 weeks revealed that the primate retina responds to defocus of different signs by activation or suppression of largely distinct pathways. We also found that 29 genes differentially expressed in the marmoset retina in response to imposed defocus are localized within human myopia quantitative trait loci (QTLs), suggesting functional overlap between genes differentially expressed in the marmoset retina upon exposure to optical defocus and genes causing myopia in humans. These findings identify retinal pathways involved in the development of myopia, as well as potential new strategies for its treatment.

摘要

近视(远视)是最常见的眼部疾病,由于近年来患病率急剧上升,它已迅速成为世界上一些地区视力丧失的主要原因之一。近距工作会导致视网膜远视光学离焦,被认为是导致人类近视的环境风险因素之一。实验研究表明,放置在眼前的负球镜所产生的远视离焦会加速眼球生长并导致近视,而正镜所产生的近视离焦则会减缓眼球生长并导致折射状态产生补偿性远视偏移。这两种光学信号之间的平衡被认为可以调节屈光眼的发育;然而,视网膜识别光学离焦信号的能力以及指导正视化的分子信号通路的组成,是正在深入研究和争论的课题。我们发现,视网膜可以轻易地区分施加的近视和远视离焦,并确定了引导正视化的视网膜对不同离焦信号反应的关键信号通路。比较在 10 天或 5 周内接受近视或远视离焦的普通狨猴的视网膜转录组,发现灵长类动物视网膜对不同离焦信号的反应通过激活或抑制很大程度上不同的途径。我们还发现,在受施加的离焦影响后,在狨猴视网膜中差异表达的 29 个基因位于人类近视数量性状位点(QTL)内,这表明在暴露于光学离焦后,在狨猴视网膜中差异表达的基因与导致人类近视的基因之间存在功能重叠。这些发现确定了参与近视发展的视网膜途径,以及治疗近视的潜在新策略。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4f17/6177118/c1d1d8ff13c7/pbio.2006021.g001.jpg

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