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跨皮质、纹状体和下丘脑的位点及细胞类型特异性miRNA和mRNA基因与网络。

Site- and cell-type-specific miRNA and mRNA genes and networks across the cortex, striatum, and hypothalamus.

作者信息

Zacharias Amanda M, O'Connor Ciara D, Topouza Danai G, Fang Zhi Yi, Ghazinejad Helia, Chen Hanlin, Duan Qingling, Ghasemlou Nader

机构信息

Department of Biomedical and Molecular Sciences, Queen's University, Kingston, ON, Canada.

School of Computing, Queen's University, Kingston, ON, Canada.

出版信息

Commun Biol. 2025 Jul 1;8(1):969. doi: 10.1038/s42003-025-08371-7.

Abstract

Biological rhythms control gene expression, but effects on central nervous system (CNS) cells and structures remain poorly defined. While circadian (24-hour) rhythms are most studied, many genes have periods of greater and less than 24-hours; these fluctuations can be both site- and cell-specific. Identifying patterns of gene rhythmicity across the CNS is necessary for both the study of chronobiology and to make sense of data obtained in the laboratory. We now identify cycling mRNAs, miRNAs, gene networks and mRNA-miRNA co-expression pairs in the cortex, hypothalamus, and corpus striatum of male C57BL/6J mice using high-dimensional datasets. A searchable catalogue ( https://www.ghasemloulab.ca/chronoCNS ) helps refine the analysis of cellular and molecular rhythmicity across the CNS (using the liver as a control). Immunofluorescence confirms the rhythmicity of key targets across cells in these structures, with strong cycling signatures in resting oligodendrocytes. Our study sheds light on the contribution of diurnal, ultradian, and infradian rhythms and mRNA-miRNA interactions to CNS function.

摘要

生物节律控制基因表达,但对中枢神经系统(CNS)细胞和结构的影响仍不清楚。虽然昼夜(24小时)节律研究最多,但许多基因的周期大于或小于24小时;这些波动可能因部位和细胞而异。识别整个中枢神经系统的基因节律模式对于生物钟学研究以及理解实验室获得的数据都很有必要。我们现在使用高维数据集,在雄性C57BL/6J小鼠的皮层、下丘脑和纹状体中识别循环mRNA、miRNA、基因网络和mRNA-miRNA共表达对。一个可搜索的目录(https://www.ghasemloulab.ca/chronoCNS )有助于完善对整个中枢神经系统细胞和分子节律的分析(以肝脏作为对照)。免疫荧光证实了这些结构中关键靶点在细胞间的节律性,在静息少突胶质细胞中有强烈的循环信号。我们的研究揭示了昼夜节律、超日节律和亚日节律以及mRNA-miRNA相互作用对中枢神经系统功能的贡献。

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