Mapping the daily rhythmic transcriptome in the diabetic retina

IF 1.5 4区 心理学 Q4 NEUROSCIENCES
Ryan P. Silk , Hanagh R. Winter , Ouria Dkhissi-Benyahya , Carmella Evans-Molina , Alan W. Stitt , Vijay K. Tiwari , David A. Simpson , Eleni Beli
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Abstract

Retinal function changes dramatically from day to night, yet clinical diagnosis, treatments, and experimental sampling occur during the day. To begin to address this gap in our understanding of disease pathobiology, this study investigates whether diabetes affects the retina's daily rhythm of gene expression. Diabetic, Ins2Akita/J mice, and non-diabetic littermates were kept under a 12 h:12 h light/dark cycle until 4 months of age. mRNA sequencing was conducted in retinas collected every 4 h throughout the 24 hr light/dark cycle. Computational approaches were used to detect rhythmicity, predict acrophase, identify differential rhythmic patterns, analyze phase set enrichment, and predict upstream regulators. The retinal transcriptome exhibited a tightly regulated rhythmic expression with a clear 12-hr transcriptional axis. Day-peaking genes were enriched for DNA repair, RNA splicing, and ribosomal protein synthesis, night-peaking genes for metabolic processes and growth factor signaling. Although the 12-hr transcriptional axis is retained in the diabetic retina, it is phase advanced for some genes. Upstream regulator analysis for the phase-shifted genes identified oxygen-sensing mechanisms and HIF1alpha, but not the circadian clock, which remained in phase with the light/dark cycle. We propose a model in which, early in diabetes, the retina is subjected to an internal desynchrony with the circadian clock and its outputs are still light-entrained whereas metabolic pathways related to neuronal dysfunction and hypoxia are phase advanced. Further studies are now required to evaluate the chronic implications of such desynchronization on the development of diabetic retinopathy.

Abstract Image

绘制糖尿病视网膜中每日节律性转录组
从白天到晚上,视网膜功能发生了巨大的变化,但临床诊断、治疗和实验取样都是在白天进行的。为了开始解决我们对疾病病理生物学理解中的这一差距,本研究调查了糖尿病是否影响视网膜的日常基因表达节奏。将糖尿病小鼠、Ins2Akita/J小鼠和非糖尿病小鼠置于12小时:12小时的明暗循环中,直到4个月大。在24小时光照/黑暗周期中,每4小时采集一次视网膜进行mRNA测序。计算方法用于检测节律性,预测顶相,识别差异节律模式,分析相集富集,并预测上游调节。视网膜转录组表现出严格调控的节律性表达,具有清晰的12小时转录轴。白天峰值基因富集于DNA修复、RNA剪接和核糖体蛋白合成,夜间峰值基因富集于代谢过程和生长因子信号传导。虽然12小时的转录轴在糖尿病视网膜中保留,但对一些基因来说,它是晚期的。对相移基因的上游调控分析发现了氧传感机制和HIF1alpha,但没有发现昼夜节律钟,昼夜节律钟与光/暗周期保持一致。我们提出了一种模型,在糖尿病早期,视网膜受到与生物钟的内部不同步,其输出仍然是光携带的,而与神经元功能障碍和缺氧相关的代谢途径则处于阶段晚期。现在需要进一步的研究来评估这种非同步化对糖尿病视网膜病变发展的慢性影响。
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来源期刊
Vision Research
Vision Research 医学-神经科学
CiteScore
3.70
自引率
16.70%
发文量
111
审稿时长
66 days
期刊介绍: Vision Research is a journal devoted to the functional aspects of human, vertebrate and invertebrate vision and publishes experimental and observational studies, reviews, and theoretical and computational analyses. Vision Research also publishes clinical studies relevant to normal visual function and basic research relevant to visual dysfunction or its clinical investigation. Functional aspects of vision is interpreted broadly, ranging from molecular and cellular function to perception and behavior. Detailed descriptions are encouraged but enough introductory background should be included for non-specialists. Theoretical and computational papers should give a sense of order to the facts or point to new verifiable observations. Papers dealing with questions in the history of vision science should stress the development of ideas in the field.
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