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Bmal1 基因敲除小鼠可促进其适应光照/黑暗环境紊乱。

Bmal1 deletion in mice facilitates adaptation to disrupted light/dark conditions.

机构信息

School of Bioengineering, Dalian University of Technology, Dalian, Liaoning, China.

Institute for Translational Medicine and Therapeutics, Perelman School of Medicine, University of Pennsylvania, Philadelphia, Pennsylvania, USA.

出版信息

JCI Insight. 2019 Apr 11;5(10):125133. doi: 10.1172/jci.insight.125133.

Abstract

Recently, by utilizing conventional and tamoxifen inducible Bmal1 (Brain and muscle Arnt-like protein 1) knockout mice, we found that delaying the loss of circadian rhythms to adulthood attenuates the impact on general integrity and survival at least under 12h light/12h dark conditions (LD). To understand further the contribution of Bmal1 in post-natal life under conditions of circadian disruption, we subjected inducible knockout mice (KO) and their littermate controls (Ctrl) to forced desynchrony protocols including cycles with non-24h periods, randomized light/dark cycles, and jet lag, and monitored their locomotor activity using radiotelemetry. Under these conditions, control mice cannot be entrained, as reflected by their maintenance of circadian behavior irrespective of schedules. By contrast, KO mice displayed higher activity levels in the dark phases of most cycles. Under a 3h light/3h dark regime, Ctrls displayed higher activity levels in the dark phases of all cycles although there were still obvious circadian rhythms, suggesting that an ultradian mechanism is also involved. Insulin sensitivity was markedly reduced by disrupted light schedules as expected in Ctrls, but not in the KOs. Thus, Bmal1 deletion in adult mice facilitates adaptation to new light/dark schedules and protects from insulin resistance induced by circadian disruption.

摘要

最近,通过利用常规和他莫昔芬诱导的 Bmal1(脑和肌肉芳香烃受体核蛋白 1)敲除小鼠,我们发现将昼夜节律的丧失延迟到成年期可以减轻其对整体完整性和生存的影响,至少在 12 小时光照/12 小时黑暗条件(LD)下是这样。为了进一步了解 Bmal1 在昼夜节律紊乱的出生后生活中的作用,我们对诱导型敲除小鼠(KO)及其同窝对照(Ctrl)进行了强制去同步化方案的实验,包括非 24 小时周期、随机光照/黑暗周期和时差,并用无线电遥测术监测它们的活动。在这些条件下,由于不受时间表的影响,对照小鼠的昼夜行为仍保持不变,因此无法被重新同步。相比之下,KO 小鼠在大多数周期的黑暗阶段表现出更高的活动水平。在 3 小时光照/3 小时黑暗的方案下,Ctrl 在所有周期的黑暗阶段显示出更高的活动水平,尽管仍存在明显的昼夜节律,这表明超昼夜机制也参与其中。如预期的那样,光照时间表的打乱会导致对照小鼠的胰岛素敏感性明显降低,但 KO 小鼠则不会。因此,成年小鼠中 Bmal1 的缺失促进了对新的光照/黑暗时间表的适应,并防止了由昼夜节律紊乱引起的胰岛素抵抗。

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