成年小鼠睡眠的体细胞遗传学分析。

IF 0.2 4区化学 Q4 CHEMISTRY, ANALYTICAL Bunseki Kagaku Pub Date : 2022-07-13 DOI:10.1523/JNEUROSCI.0089-22.2022

Guodong Wang, Qi Li, Junjie Xu, Shuai Zhao, Rui Zhou, Zhenkang Chen, Wentong Jiang, Xue Gao, Shuang Zhou, Zhiyu Chen, Quanzhi Sun, Chengyuan Ma, Lin Chen, Bihan Shi, Ying Guo, Haiyan Wang, Xia Wang, Huaiye Li, Tao Cai, Yibing Wang, Zhineng Chen, Fengchao Wang, Qinghua Liu

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引用次数: 0

摘要

经典的小鼠正向和反向遗传需要种系突变，因此对于研究重要基因或冗余通路的睡眠功能来说并不方便。此外，由于手术和基因杂交耗费大量人力，基于脑电图/肌电图进行小鼠睡眠筛查也非常耗时。在这里，我们描述了一种高度精确的 SleepV（视频）系统和基于腺相关病毒（AAV）的成体脑嵌合体（ABC）表达/基因敲除（KO）平台，用于对成年雄性或雌性小鼠的睡眠进行体细胞遗传学分析。试验性 ABC 筛选发现了 CREB 和 CRTC1，它们的组成型或诱导型表达会显著降低非快速眼动睡眠的数量和/或质量。通过AAV-Cre注射Sik3-E13flox/flox成年小鼠Sik3外显子13的ABC-KO可使嗜睡（Sik3Slp/+）小鼠表型复制，而Slp/Sik3的ABC-CRISPR可逆转嗜睡小鼠的嗜睡症，表明SLP/SIK3激酶在睡眠调节中的直接作用。对奥曲肽/视黄醇受体进行多重 ABC-CRISPR 可导致嗜睡症发作，从而实现了对成年小鼠冗余基因的一步分析。因此，这种体细胞遗传学方法可以跳过小鼠的发育过程，最大限度地减少基因杂交，从而促进对成年小鼠睡眠调控基因的高通量分析，尤其是对重要或冗余基因的分析。经典的种系小鼠遗传学对于研究重要基因或冗余通路的睡眠功能非常不便。基于脑电图（EEG）/脑电图（EMG）的小鼠睡眠筛选耗时长，因为需要进行劳动密集型手术和漫长的基因杂交。为了克服这些 "瓶颈"，我们开发了基于视频的高精度睡眠分析系统和腺相关病毒介导的 ABC 表达/基因敲除平台，用于成年小鼠睡眠的体细胞遗传学分析。这些方法不仅有助于快速鉴定睡眠调控基因，还有助于对小鼠睡眠调控的分子途径进行高效的机理研究。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Somatic Genetics Analysis of Sleep in Adult Mice.

Classical forward and reverse mouse genetics require germline mutations and, thus, are unwieldy to study sleep functions of essential genes or redundant pathways. It is also time-consuming to conduct EEG/EMG-based mouse sleep screening because of labor-intensive surgeries and genetic crosses. Here, we describe a highly accurate SleepV (video) system and adeno-associated virus (AAV)-based adult brain chimeric (ABC)-expression/KO platform for somatic genetics analysis of sleep in adult male or female mice. A pilot ABC screen identifies CREB and CRTC1, of which constitutive or inducible expression significantly reduces quantity and/or quality of non-rapid eye movement sleep. Whereas ABC-KO of exon 13 of Sik3 by AAV-Cre injection in Sik3-E13^flox/flox adult mice phenocopies Sleepy (Sik3 ^Slp/+ ) mice, ABC-CRISPR of Slp/Sik3 reverses hypersomnia of Sleepy mice, indicating a direct role of SLP/SIK3 kinase in sleep regulation. Multiplex ABC-CRISPR of both orexin/hypocretin receptors causes narcolepsy episodes, enabling one-step analysis of redundant genes in adult mice. Therefore, this somatic genetics approach should facilitate high-throughput analysis of sleep regulatory genes, especially for essential or redundant genes, in adult mice by skipping mouse development and minimizing genetic crosses.SIGNIFICANCE STATEMENT The molecular mechanisms of mammalian sleep regulation remain unclear. Classical germline mouse genetics are unwieldy to study sleep functions of essential genes or redundant pathways. The EEG/EMG-based mouse sleep screening is time-consuming because of labor-intensive surgeries and lengthy genetic crosses. To overcome these "bottlenecks," we developed a highly accurate video-based sleep analysis system and adeno-associated virus-mediated ABC-expression/KO platform for somatic genetics analysis of sleep in adult mice. These methodologies facilitate rapid identification of sleep regulatory genes, but also efficient mechanistic studies of the molecular pathways of sleep regulation in mice.

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来源期刊

Bunseki Kagaku 化学-分析化学

CiteScore

0.30

自引率

0.00%

发文量

审稿时长

3 months

期刊介绍： Bunsekikagaku is a journal written in Japanese and is published monthly by The Japan Society for Analytical Chemistry. The journal publishes papers on all aspects of the theory and practice of analytical sciences, including fundamental and applied, inorganic and organic, wet chemical and instrumental methods.