Circadian regulation of microRNA-target chimeras in Drosophila

生物 小RNA 昼夜节律 基因沉默 生物钟 阿尔戈瑙特 细胞生物学 遗传学 基因 核糖核酸 RNA干扰 神经科学
作者
Xiju Xia,Xiaonan Fu,Binbin Wu,Jinsong Zhu,Zhangwu Zhao
标识
DOI:10.1101/622183
摘要

Abstract MicroRNA is critical coordinator to circadian regulation by silencing gene expression. Although many circadian related miRNAs and some of its target are known, the global functional miRNA-mRNA interaction networks remain poorly understand which is hindered by imperfect base-pairing between miRNA and target mRNA. In this study, we used CLEAR (Covalent Ligation of Endogenous Argonaute-bound RNAs) -CLIP (Cross-Linking and Immuno-Precipitation) to explore the regulatory functions of miRNAs in the circadian system by comparing the miRNA-mRNA interactions between the Drosophila wild-type strain w 1118 and the Clk mutant Clk jrk . We unambiguously identified thousands of miRNA-mRNA interactions from CLEAR-CLIP data set at unprecedented depth in vivo for the first time. Among them, about 300 miRNA-mRNA interactions were involved in the regulation of circadian, in which miRNAs targeting core clock genes pdp1 , tim and vri presented distinct changes in response to Clk jrk . Particularly, the mir-375-timeless interaction from CLER-CLIP shows important effects on circadian, this functional event occurred in the l-LNv neurons. Overexpression of mir-375 in tim neurons caused decreases in TIM content resulting in arrhythmicity of daily locomotion and changes of sleep. This present work provides a global view of miRNA targeting in the circadian rhythm.

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