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BTBR小鼠对光的昼夜节律反应。

Circadian Responses to Light in the BTBR Mouse.

作者信息

Vijaya Shankara Jhenkruthi, Horsley Katelyn G, Cheng Ning, Rho Jong M, Antle Michael C

机构信息

Department of Psychology, University of Calgary, Calgary, AB, Canada.

Hotchkiss Brain Institute, Cumming School of Medicine, University of Calgary, Calgary, AB, Canada.

出版信息

J Biol Rhythms. 2022 Oct;37(5):498-515. doi: 10.1177/07487304221102279. Epub 2022 Jun 20.

Abstract

Animals with altered freerunning periods are valuable in understanding properties of the circadian clock. Understanding the relationship between endogenous clock properties, entrainment, and influence of light in terms of parametric and non-parametric models can help us better understand how different populations adapt to external light cycles. Many clinical populations often show significant changes in circadian properties that in turn cause sleep and circadian problems, possibly exacerbating their underlying clinical condition. BTBR TItpr3/J (BTBR) mice are a model commonly used for the study of autism spectrum disorders (ASD). Adults and adolescents with ASD frequently exhibit profound sleep and circadian disruptions, including increased latency to sleep, insomnia, advanced and delayed sleep phase disorders, and sleep fragmentation. Here, we investigated the circadian phenotype of BTBR mice in freerunning and light-entrained conditions and found that this strain of mice showed noticeably short freerunning periods (~22.75 h). In addition, when compared to C57BL/6J controls, BTBR mice also showed higher levels of activity even though this activity was compressed into a shorter active phase. Phase delays and phase advances to light were significantly larger in BTBR mice. Despite the short freerunning period, BTBR mice exhibited normal entrainment in light-dark cycles and accelerated entrainment to both advanced and delayed light cycles. Their ability to entrain to skeleton photoperiods of 1 min suggests that this entrainment cannot be attributed to masking. Period differences were also correlated with differences in the number of vasoactive intestinal polypeptide-expressing cells in the suprachiasmatic nucleus (SCN). Overall, the BTBR model, with their unique freerunning and entrainment properties, makes an interesting model to understand the underlying circadian clock.

摘要

自由活动周期改变的动物对于理解昼夜节律钟的特性很有价值。从参数模型和非参数模型的角度理解内源性生物钟特性、昼夜节律调节以及光照影响之间的关系,有助于我们更好地了解不同群体如何适应外部光照周期。许多临床群体常常表现出昼夜节律特性的显著变化,进而导致睡眠和昼夜节律问题,这可能会加重他们潜在的临床病症。BTBR TItpr3/J(BTBR)小鼠是常用于研究自闭症谱系障碍(ASD)的模型。患有ASD的成年人和青少年经常表现出严重的睡眠和昼夜节律紊乱,包括入睡潜伏期延长、失眠、睡眠相位提前和延迟障碍以及睡眠碎片化。在此,我们研究了BTBR小鼠在自由活动和光照调节条件下的昼夜节律表型,发现该品系小鼠的自由活动周期明显较短(约22.75小时)。此外,与C57BL/6J对照组相比,BTBR小鼠即使其活动被压缩到较短的活跃期,仍表现出更高的活动水平。BTBR小鼠对光照的相位延迟和相位提前明显更大。尽管自由活动周期较短,但BTBR小鼠在明暗周期中表现出正常的昼夜节律调节,并且对提前和延迟的光照周期都能加速昼夜节律调节。它们对1分钟骨架光周期的昼夜节律调节能力表明,这种昼夜节律调节不能归因于掩盖效应。周期差异也与视交叉上核(SCN)中表达血管活性肠肽的细胞数量差异相关。总体而言,BTBR模型具有独特的自由活动和昼夜节律调节特性,是一个理解潜在昼夜节律钟的有趣模型。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7301/9452857/1c7e65ff80f3/10.1177_07487304221102279-fig1.jpg

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