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Characterizing Light-Regulated Retinal MicroRNAs Reveals Rapid Turnover as a Common Property of Neuronal MicroRNAs

机译:表征光调节性视网膜MicroRNA揭示了快速周转作为神经元MicroRNA的共同特性。

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Adaptation to different levels of illumination is central to the function of the retina. Here, we demonstrate that levels of the miR-183/96/182 cluster, miR-204, and miR-211 are regulated by different light levels in the mouse retina. Concentrations of these microRNAs were downregulated during dark adaptation and upregulated in light-adapted retinas, with rapid decay and increased transcription being responsible for the respective changes. We identified the voltage-dependent glutamate transporter Slc1a1 as one of the miR-183/96/182 targets in photoreceptor cells. We found that microRNAs in retinal neurons decay much faster than microRNAs in nonneuronal cells. The high turnover is also characteristic of microRNAs in hippocampal and cortical neurons, and neurons differentiated from ES cells in vitro. Blocking activity reduced turnover of microRNAs in neuronal cells while stimulation with glutamate accelerated it. Our results demonstrate that microRNA metabolism in neurons is higher than in most other cells types and linked to neuronal activity.
机译:适应不同水平的照明对于视网膜的功能至关重要。在这里,我们证明了miR-183 / 96/182簇,miR-204和miR-211的水平受小鼠视网膜中不同光水平的调节。这些microRNA的浓度在黑暗适应过程中被下调,而在光适应性视网膜中被上调,其中快速衰减和转录增加是相应变化的原因。我们确定了电压依赖性谷氨酸转运蛋白Slc1a1作为感光细胞中的miR-183 / 96/182目标之一。我们发现,视网膜神经元中的microRNA比非神经元细胞中的microRNA衰减快得多。高周转率也是海马和皮层神经元以及体外从ES细胞分化出来的神经元中microRNA的特征。阻断活性减少了神经元细胞中microRNA的转换,而谷氨酸刺激加速了它的转换。我们的结果表明,神经元中的microRNA代谢高于大多数其他细胞类型,并且与神经元活性有关。

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