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首页> 外文期刊>Journal of biomedicine & biotechnology >Characterization of phototransduction gene knockouts revealed important signaling networks in the light-induced retinal degeneration.
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Characterization of phototransduction gene knockouts revealed important signaling networks in the light-induced retinal degeneration.

机译:光转基因基因敲除的表征揭示了光诱导的视网膜变性中的重要信号网络。

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摘要

Understanding the molecular pathways mediating neuronal function in retinas can be greatly facilitated by the identification of genes regulated in the retinas of different mutants under various light conditions. We attempted to conduct a gene chip analysis study on the genes regulated during rhodopsin kinase (Rhok-/-) and arrestin (Sag-/-) knockout and double knockouts in mice retina. Hence, mice were exposed to constant illumination of 450 lux or 6,000 lux on dilated pupils for indicated periods. The retinas were removed after the exposure and processed for microarray analysis. Double knockout was associated with immense changes in gene expression regulating a number of apoptosis inducing transcription factors. Subsequently, network analysis revealed that during early exposure the transcription factors, p53, c-MYC, c-FOS, JUN, and, in late phase, NFkappaB, appeared to be essential for the initiation of light-induced retinal rod loss, and some other classical pro- and antipoptotic genes appeared to be significantly important as well.
机译:通过鉴定在各种光照条件下不同突变体的视网膜中调控的基因,可以大大促进理解介导视网膜神经元功能的分子途径。我们试图对小鼠视网膜中视紫红质激酶(Rhok-/-)和抑制素(Sag-/-)敲除和双敲除过程中调控的基因进行基因芯片分析研究。因此,在指定的时间段内,使小鼠在散瞳上持续暴露于450 lux或6,000 lux的光照下。暴露后去除视网膜,并进行微阵列分析。双重敲除与调节许多凋亡诱导转录因子的基因表达的巨大变化有关。随后,网络分析表明,在早期暴露过程中,转录因子p53,c-MYC,c-FOS,JUN和晚期NFkappaB似乎是引发光诱导的视网膜棒丢失的必要条件,其中一些其他经典的促凋亡和抗凋亡基因似乎也非常重要。

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