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应用于睡眠研究的演化发育生物学:一个时机已至的方法。

Evo-devo applied to sleep research: an approach whose time has come.

作者信息

Brown Ritchie E

机构信息

Department of Psychiatry, VA Boston Healthcare System and Harvard Medical School, West Roxbury, MA, USA.

出版信息

Sleep Adv. 2024 Jun 15;5(1):zpae040. doi: 10.1093/sleepadvances/zpae040. eCollection 2024.

Abstract

Sleep occurs in all animals but its amount, form, and timing vary considerably between species and between individuals. Currently, little is known about the basis for these differences, in part, because we lack a complete understanding of the brain circuitry controlling sleep-wake states and markers for the cell types which can identify similar circuits across phylogeny. Here, I explain the utility of an "Evo-devo" approach for comparative studies of sleep regulation and function as well as for sleep medicine. This approach focuses on the regulation of evolutionary ancient transcription factors which act as master controllers of cell-type specification. Studying these developmental transcription factor cascades can identify novel cell clusters which control sleep and wakefulness, reveal the mechanisms which control differences in sleep timing, amount, and expression, and identify the timepoint in evolution when different sleep-wake control neurons appeared. Spatial transcriptomic studies, which identify cell clusters based on transcription factor expression, will greatly aid this approach. Conserved developmental pathways regulate sleep in mice, , and . Members of the LIM Homeobox () gene family control the specification of sleep and circadian neurons in the forebrain and hypothalamus. Increased activity may account for increased orexin/hypocretin neurons and reduced sleep in Mexican cavefish. Other transcription factor families specify sleep-wake circuits in the brainstem, hypothalamus, and basal forebrain. The expression of transcription factors allows the generation of specific cell types for transplantation approaches. Furthermore, mutations in developmental transcription factors are linked to variation in sleep duration in humans, risk for restless legs syndrome, and sleep-disordered breathing. This paper is part of the "Genetic and other molecular underpinnings of sleep, sleep disorders, and circadian rhythms including translational approaches" collection.

摘要

所有动物都会睡眠,但睡眠的时长、形式和时间安排在物种之间以及个体之间存在很大差异。目前,对于这些差异的基础我们知之甚少,部分原因在于我们尚未完全理解控制睡眠 - 觉醒状态的脑回路以及能够在系统发育中识别相似回路的细胞类型标记物。在此,我解释一种“进化发育(Evo - devo)”方法在睡眠调节与功能的比较研究以及睡眠医学中的作用。这种方法聚焦于对进化上古老的转录因子的调控,这些转录因子充当细胞类型特化的主控因子。研究这些发育转录因子级联反应能够识别出控制睡眠和觉醒的新型细胞簇,揭示控制睡眠时间、时长和表现差异的机制,并确定不同睡眠 - 觉醒控制神经元出现的进化时间点。基于转录因子表达来识别细胞簇的空间转录组学研究将极大地助力这一方法。保守的发育途径在小鼠中调节睡眠。LIM 同源框(LIM Homeobox,Lhx)基因家族的成员控制前脑和下丘脑中睡眠和昼夜节律神经元的特化。Lhx 活性增加可能是墨西哥脂鲤中食欲素/下丘泌素神经元增加以及睡眠减少的原因。其他转录因子家族则确定脑干、下丘脑和基底前脑中的睡眠 - 觉醒回路。转录因子的表达使得能够生成用于移植方法的特定细胞类型。此外,发育转录因子的突变与人类睡眠时长的变化、不安腿综合征的风险以及睡眠呼吸障碍有关。本文是“睡眠、睡眠障碍和昼夜节律的遗传及其他分子基础,包括转化方法”系列文章的一部分。

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