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Postnatal Constant Light Compensates Cryptochrome1 and 2 Double Deficiency for Disruption of Circadian Behavioral Rhythms in Mice under Constant Dark

机译:产后恒光补偿Cryptochrome1和2双重缺陷对恒暗条件下小鼠昼夜行为节奏的破坏。

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摘要

Clock genes Cryptochrome (Cry1) and Cry2 are essential for expression of circadian rhythms in mice under constant darkness (DD). However, circadian rhythms in clock gene Per1 expression or clock protein PER2 are detected in the cultured suprachiasmatic nucleus (SCN) of neonatal Cry1 and Cry2 double deficient (Cry1-/-/Cry2-/-) mice. A lack of circadian rhythms in adult Cry1-/-/Cry2-/- mice is most likely due to developmentally disorganized cellular coupling of oscillating neurons in the SCN. On the other hand, neonatal rats exposed to constant light (LL) developed a tenable circadian system under prolonged LL which was known to fragment circadian behavioral rhythms. In the present study, Cry1-/-/Cry2-/- mice were raised under LL from postnatal day 1 for 7 weeks and subsequently exposed to DD for 3 weeks. Spontaneous movement was monitored continuously after weaning and PER2::LUC was measured in the cultured SCN obtained from mice under prolonged DD. Surprisingly, Chi square periodogram analysis revealed significant circadian rhythms of spontaneous movement in the LL-raised Cry1-/-/Cry2-/- mice, but failed to detect the rhythms in Cry1-/-/Cry2-/- mice raised under light-dark cycles (LD). By contrast, prolonged LL in adulthood did not rescue the circadian behavioral rhythms in the LD raised Cry1-/-/Cry2-/- mice. Visual inspection disclosed two distinct activity components with different periods in behavioral rhythms of the LL-raised Cry1-/-/Cry2-/- mice under DD: one was shorter and the other was longer than 24 hours. The two components repeatedly merged and separated. The patterns resembled the split behavioral rhythms of wild type mice under prolonged LL. In addition, circadian rhythms in PER2::LUC were detected in some of the LL-raised Cry1-/-/Cry2-/- mice under DD. These results indicate that neonatal exposure to LL compensates the CRY double deficiency for the disruption of circadian behavioral rhythms under DD in adulthood.
机译:时钟基因Cryptochrome(Cry1)和Cry2对于在恒定黑暗(DD)下小鼠中昼夜节律的表达至关重要。但是,在新生的Cry1和Cry2双缺陷(Cry1-/-// Cry2-/-)小鼠的视交叉上核(SCN)中检测到了时钟基因Per1表达或时钟蛋白PER2的昼夜节律。成年Cry1-/-/ Cry2-/-小鼠缺乏昼夜节律是由于SCN中振荡神经元的发育紊乱的细胞偶联所致。另一方面,暴露于恒定光(LL)的新生大鼠在延长的LL下发展了一个稳定的昼夜节律系统,这已知会破坏昼夜节律的行为节律。在本研究中,Cry1-/-// Cry2-/-小鼠从出生后第1天起在LL下饲养7周,然后暴露于DD 3周。断奶后连续监测自发运动,并在延长的DD下测量从小鼠获得的培养SCN中的PER2 :: LUC。出乎意料的是,卡方平方图分析显示在LL升高的Cry1-/-// Cry2-/-小鼠中自发运动有明显的昼夜节律,但未能检测到在光照下饲养的Cry1-/-// Cry2-/-小鼠的节律。黑暗周期(LD)。相比之下,成年期延长的LL不能挽救LD饲养的Cry1-/-/ Cry2-/-小鼠的昼夜节律行为节律。视觉检查揭示了在DD下LL饲养的Cry1-/-// Cry2-/-小鼠的行为节律有两个不同的活动周期,这些活动周期不同:一个较短,而另一个长于24小时。这两个组成部分反复合并和分离。该模式类似于在延长的LL下野生型小鼠的分裂行为节律。此外,在DD下,一些LL升高的Cry1-/-/ Cry2-/-小鼠中检测到PER2 :: LUC中的昼夜节律。这些结果表明,新生儿暴露于LL可以弥补成年DD引起的昼夜节律行为节律紊乱的CRY双重缺陷。

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