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褪黑素充足(C3H)和褪黑素缺乏(C57BL)小鼠视网膜中的生物钟基因表达。

Clock gene expression in the retina of melatonin-proficient (C3H) and melatonin-deficient (C57BL) mice.

作者信息

Dinet Virginie, Ansari Nariman, Torres-Farfan Claudia, Korf Horst-Werner

机构信息

Dr Senckenbergische Anatomie, Institut für Anatomie II, Johann Wolfgang Goethe-Universität Frankfurt, Frankfurt am Main, Frankfurt, Germany.

出版信息

J Pineal Res. 2007 Jan;42(1):83-91. doi: 10.1111/j.1600-079X.2006.00387.x.

Abstract

In several mammalian species, the retina contains an autonomous circadian clock and is capable of synthesizing melatonin. The function of circadian clocks depends on interlocking transcriptional/translational feedback loops involving several clock genes. Here we investigated the expression of two clock genes (Per1, Cry2) and the level of phosphorylated (p) cyclic AMP response element binding protein (CREB) in retinae of melatonin-deficient (C57BL) with an intact retina and melatonin-proficient (C3H) mice with degenerated outer nuclear layer. RNase protection assay and in situ hybridization revealed in both strains a rhythm in transcript levels for Per1 with a peak at zeitgeber time (ZT) 08, but not for Cry2. Immunoreactions for PER1, CRY2 and pCREB were localized to the nuclei of cells in the inner nuclear layer (INL) and ganglion cell layer (GC) of both strains and to the outer nuclear layer of C57BL. In C3H, protein levels of PER1 and CRY2 followed a clear day/night rhythm in the INL and the GC with a peak at the end of the day (ZT14). pCREB levels peaked at the beginning of the day. Noteably, in melatonin-deficient C57BL mice, protein levels of PER1, CRY2 and pCREB did not show significant changes over a 16L/8D cycle. These data suggest that melatonin influences PER1 and CRY2 protein levels via post-transcriptional mechanisms and also plays a role in rhythmic regulation of pCREB levels in the mammalian retina.

摘要

在几种哺乳动物物种中,视网膜含有一个自主的生物钟,并且能够合成褪黑素。生物钟的功能取决于涉及多个时钟基因的相互连锁的转录/翻译反馈环。在此,我们研究了褪黑素缺乏(C57BL)且视网膜完整的小鼠以及褪黑素充足(C3H)但外核层退化的小鼠视网膜中两个时钟基因(Per1、Cry2)的表达以及磷酸化(p)环磷酸腺苷反应元件结合蛋白(CREB)的水平。核糖核酸酶保护分析和原位杂交显示,在这两个品系中,Per1的转录水平均呈现节律性,在授时时间(ZT)08达到峰值,但Cry2没有。PER1、CRY2和pCREB的免疫反应定位于两个品系内核层(INL)和神经节细胞层(GC)细胞的细胞核以及C57BL的外核层。在C3H中,INL和GC中PER1和CRY2的蛋白质水平呈现明显的昼夜节律,在一天结束时(ZT14)达到峰值。pCREB水平在一天开始时达到峰值。值得注意的是,在褪黑素缺乏的C57BL小鼠中,PER1、CRY2和pCREB的蛋白质水平在16小时光照/8小时黑暗周期内没有显著变化。这些数据表明,褪黑素通过转录后机制影响PER1和CRY2的蛋白质水平,并且在哺乳动物视网膜中pCREB水平的节律性调节中也发挥作用。

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