Hunt for mammalian sleep-regulating genes

Hiromasa Funato, Masashi Yanagisawa
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引用次数: 2

Abstract

Genetics is one of the various approaches adopted to understand and control mammalian sleep. Reverse genetics, which is usually applied to analyze sleep in gene-deficient mice, has been the mainstream field of genetic studies on sleep for the past three decades and has revealed that various molecules, including orexin, are involved in sleep regulation. Recently, forward genetic studies in humans and mice have identified gene mutations responsible for heritable sleep abnormalities, such as SIK3, NALCN, DEC2, the neuropeptide S receptor, and β1 adrenergic receptor. Furthermore, the protein kinase A-SIK3 pathway was shown to represent the intracellular neural signaling for sleep need. Large-scale genome-wide analyses of human sleep have been conducted, and many gene loci associated with individual differences in sleep have been found. The development of genome-editing technology and gene transfer by an adeno-associated virus has updated and expanded the genetic studies on mammals. These efforts are expected to elucidate the mechanisms of sleep–wake regulation and develop new therapeutic interventions for sleep disorders.
寻找哺乳动物睡眠调节基因
遗传学是用来理解和控制哺乳动物睡眠的多种方法之一。反向遗传学通常用于分析基因缺陷小鼠的睡眠,在过去三十年中一直是睡眠基因研究的主流领域,并揭示了包括食欲素在内的各种分子参与睡眠调节。最近,在人类和小鼠中进行的遗传学研究已经确定了导致遗传性睡眠异常的基因突变,如SIK3、NALCN、DEC2、神经肽S受体和β1肾上腺素能受体。此外,蛋白激酶A-SIK3通路被证明代表睡眠需要的细胞内神经信号。人们对人类睡眠进行了大规模的全基因组分析,发现了许多与睡眠个体差异相关的基因位点。基因组编辑技术和腺相关病毒基因转移的发展更新和扩大了对哺乳动物的遗传研究。这些努力有望阐明睡眠-觉醒调节的机制,并为睡眠障碍开发新的治疗干预措施。
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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