Damiani Devid, Alexander John J, O'Rourke Jason R, McManus Mike, Jadhav Ashutosh P, Cepko Constance L, Hauswirth William W, Harfe Brian D, Strettoi Enrica
Neuroscience Institute, Italian National Research Council, 56100 Pisa, Italy.
J Neurosci. 2008 May 7;28(19):4878-87. doi: 10.1523/JNEUROSCI.0828-08.2008.
MicroRNAs (miRNAs) are small, highly conserved molecules that have been shown to regulate the expression of genes by binding to specific target mRNAs. Dicer, an RNase III endonuclease, is essential for the production and function of mature miRNAs, and removal of Dicer has been shown to disrupt many developmental processes. In this study, Dicer was removed specifically from the retina using a floxed Dicer conditional allele and the retinal Chx10Cre transgene. Retinal Dicer knock-out mice displayed a reproducible inability to respond to light. In addition, morphological defects were observed with the formation of photoreceptor rosettes at postnatal day 16, which progressed to more general cellular disorganization and widespread degeneration of retinal cell types as the animals aged. This was accompanied by concomitant decrease in both scotopic and photopic electroretinogram (ERG) responses. Interestingly, removing a single allele of Dicer resulted in ERG deficits throughout life but not to morphological abnormalities. Northern blot analysis of Dicer-depleted retinas showed a decrease in several miRNAs. The observation that progressive retinal degeneration occurred after removal of Dicer raises the possibility that miRNAs are involved in retinal neurodegenerative disorders.
微小RNA(miRNA)是一类小的、高度保守的分子,已证明其通过与特定的靶mRNA结合来调控基因表达。Dicer是一种核糖核酸酶III内切核酸酶,对成熟miRNA的产生和功能至关重要,并且已证明去除Dicer会破坏许多发育过程。在本研究中,利用携带floxed Dicer条件等位基因和视网膜Chx10Cre转基因,特异性地从视网膜中去除Dicer。视网膜Dicer基因敲除小鼠表现出对光反应的重复性缺失。此外,在出生后第16天观察到形态学缺陷,即形成光感受器玫瑰花结,随着动物年龄增长,这种缺陷会发展为更普遍的细胞紊乱和视网膜细胞类型的广泛退化。这伴随着暗视和明视视网膜电图(ERG)反应的相应降低。有趣的是,去除Dicer的一个等位基因会导致终身ERG缺陷,但不会导致形态学异常。对Dicer缺失的视网膜进行Northern印迹分析显示几种miRNA减少。去除Dicer后发生进行性视网膜退化这一观察结果增加了miRNA参与视网膜神经退行性疾病的可能性。
