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首页> 外文期刊>Human Molecular Genetics >Segregation of expression of mPeriod gene homologs in neurons and glia: possible divergent roles of mPeriod1 and mPeriod2 in the brain
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Segregation of expression of mPeriod gene homologs in neurons and glia: possible divergent roles of mPeriod1 and mPeriod2 in the brain

机译:mPeriod基因同源物在神经元和神经胶质细胞中的表达分离:mPeriod1和mPeriod2在大脑中可能有不同的作用

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The suprachiasmatic nuclei (SCN) of the mammalian hypothalamus function as the master circadian clock, coordinating the timing of diverse cell populations and organ systems. Dysregulation of clock timing is linked to a broad range of human conditions, including obesity, cardiovascular disease and a wide spectrum of neurological disorders. Aberrant regulation of expression of the PERIOD genes has been associated with improper cell division and human cancers, while the autosomal dominant disorder familial advanced sleep phase syndrome has been mapped to a single missense mutation within the critical clock gene hPERIOD2. An essential tool to begin to dissect the inherent molecular timing process is the clock gene reporter. Here, we functionally characterize two new mouse transgenic clock reporters, mPeriod1-Venus and mPeriod2-DsRED. Venus and DsRED are fluorescent proteins that can be used to monitor transcription in individual cells in real-time. Imaging of the SCN revealed oscillations, as well as light inducibility, in Venus and DsRED expression. Rhythmic Venus and DsRED expression was observed in distinct SCN cell populations, suggesting the existence of discrete cellular SCN clocks. Outside of the SCN, mPeriod1-Venus expression was broadly expressed in neuronal and non-neuronal populations. Conversely, mPeriod2-DsRED was expressed in glial populations and progenitor cells of the dentate gyrus; limited expression was detected in neurons. This distinct expression pattern of the two reporters reveals that the central nervous system possesses mechanistically distinct subpopulations of neuronal and non-neuronal cellular clocks. These novel mouse models will facilitate our understanding of clock timing and its role in human diseases.
机译:哺乳动物下丘脑的视交叉上核(SCN)起着昼夜节律的主要作用,协调各种细胞群和器官系统的时间。时钟定时失调与多种人类疾病有关,包括肥胖,心血管疾病和多种神经系统疾病。 PERIOD基因表达的异常调节与不适当的细胞分裂和人类癌症有关,而常染色体显性遗传病家族性晚期睡眠相综合征已映射到关键时钟基因hPERIOD2内的单个错义突变。时钟基因报告子是开始剖析固有分子计时过程的重要工具。在这里,我们功能上表征两个新的小鼠转基因时钟报道基因,mPeriod1-Venus和mPeriod2-DsRED。金星和DsRED是荧光蛋白,可用于实时监测单个细胞中的转录。 SCN的成像显示出金星和DsRED表达中的振荡以及光诱导性。在不同的SCN细胞群体中观察到有节奏的维纳斯和DsRED表达,表明存在离散的细胞SCN时钟。在SCN之外,mPeriod1-Venus表达在神经元和非神经元人群中广泛表达。相反,mPeriod2-DsRED在齿状回的神经胶质细胞群和祖细胞中表达。在神经元中检测到有限的表达。两位记者的这种独特的表达方式揭示了中枢神经系统具有神经元和非神经元细胞时钟的机械学上独特的亚群。这些新颖的鼠标模型将有助于我们了解时钟定时及其在人类疾病中的作用。

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