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昼夜节律基因表达模式在视网膜和脉络膜中的差异可区分近视进展与近视起始。

Diurnal gene expression patterns in retina and choroid distinguish myopia progression from myopia onset.

机构信息

Department of Ophthalmology, Perelman School of Medicine, University of Pennsylvania, Philadelphia, Pennsylvania, United States of America.

Penn Genomics and Sequencing Core, Perelman School of Medicine, University of Pennsylvania, Philadelphia, Pennsylvania, United States of America.

出版信息

PLoS One. 2024 Jul 19;19(7):e0307091. doi: 10.1371/journal.pone.0307091. eCollection 2024.

Abstract

The world-wide prevalence of myopia (nearsightedness) is increasing, but its pathogenesis is incompletely understood. Among many putative mechanisms, laboratory and clinical findings have implicated circadian biology in the etiology of myopia. Consistent with a circadian hypothesis, we recently reported a marked variability in diurnal patterns of gene expression in two crucial tissues controlling post-natal refractive development - the retina and choroid-at the onset of form-deprivation myopia in chick, a widely studied and validated model. To extend these observations, we assayed gene expression by RNA-Seq in retina and choroid during the progression of established unilateral form-deprivation myopia of chick. We assayed gene expression every 4 hours during a single day from myopic and contralateral control eyes. Retinal and choroidal gene expression in myopic vs. control eyes during myopia progression differed strikingly at discrete times during the day. Very few differentially expressed genes occurred at more than one time in either tissue during progressing myopia. Similarly, Gene Set Enrichment Analysis pathways varied markedly by time during the day. Some of the differentially expressed genes in progressing myopia coincided with candidate genes for human myopia, but only partially corresponded with genes previously identified at myopia onset. Considering other laboratory findings and human genetics and epidemiology, these results further link circadian biology to the pathogenesis of myopia; but they also point to important mechanistic differences between the onset of myopia and the progression of established myopia. Future laboratory and clinical investigations should systematically incorporate circadian mechanisms in studying the etiology of myopia and in seeking more effective treatments to normalize eye growth in children.

摘要

全球近视(远视)的患病率正在上升,但发病机制尚不完全清楚。在许多推测的机制中,实验室和临床发现表明昼夜节律生物学与近视的病因有关。与昼夜节律假说一致,我们最近报道了在小鸡形觉剥夺性近视开始时,两个控制出生后屈光发育的关键组织——视网膜和脉络膜中的基因表达昼夜节律模式存在明显的变异性,小鸡是一种广泛研究和验证的模型。为了扩展这些观察结果,我们通过 RNA-Seq 检测了小鸡已建立的单侧形觉剥夺性近视进展过程中视网膜和脉络膜的基因表达。我们从近视和对侧对照眼每天检测基因表达 4 小时。在近视进展过程中,与对照眼相比,近视眼中的视网膜和脉络膜基因表达在白天的不同时间差异显著。在进展性近视过程中,很少有差异表达的基因在两种组织中的一个以上时间发生。同样,基因集富集分析途径在白天的不同时间也有很大差异。在进展性近视中差异表达的一些基因与人类近视的候选基因相吻合,但仅部分与以前在近视发作时确定的基因相对应。考虑到其他实验室发现和人类遗传学和流行病学,这些结果进一步将昼夜节律生物学与近视的发病机制联系起来;但它们也指出了近视发作和已建立的近视进展之间的重要机制差异。未来的实验室和临床研究应系统地将昼夜节律机制纳入研究近视的病因,并寻求更有效的治疗方法,使儿童的眼生长正常化。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a4f8/11259283/12d57a8d0736/pone.0307091.g001.jpg

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