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生物钟的遗传基础:在脉孢菌中鉴定出frq和FRQ作为生物钟组件。

The genetic basis of the circadian clock: identification of frq and FRQ as clock components in Neurospora.

作者信息

Dunlap J C, Loros J J, Aronson B D, Merrow M, Crosthwaite S, Bell-Pedersen D, Johnson K, Lindgren K, Garceau N Y

机构信息

Department of Biochemistry, Dartmouth Medical School, Hanover, NH 03755-3844, USA.

出版信息

Ciba Found Symp. 1995;183:3-17; discussion 17-25. doi: 10.1002/9780470514597.ch2.

Abstract

Genetic approaches to the identification of clock components have succeeded in two model systems, Neurospora and Drosophila. In each organism, genes identified through screens for clock-affecting mutations (frq in Neurospora, per in Drosophila) have subsequently been shown to have characteristics of central clock components: (1) mutations in each gene can affect period length and temperature compensation, two canonical characteristics of circadian systems; (2) each gene regulates the timing of its own transcription in a circadian manner; and (3) in the case of frq, constitutively elevated expression will set the phase of the clock on release into normal conditions. Despite clear genetic and molecular similarities, however, the two genes are neither molecular nor temporal homologues. The timing of peak expression is distinct in the two genes, frq expression peaking after dawn and per expression peaking near midnight. Also, although expression of per from a constitutive promoter can rescue rhythmicity in a fly lacking the gene, constitutive expression of frq will not rescue rhythmicity in Neurospora frq-null strains, and in fact causes arrhythmicity when expressed in a wild-type strain. These data suggest that frq is and/or encodes a state variable of the circadian oscillator. Recent molecular genetic analyses of frq have shed light on the origin of temperature compensation and strongly suggest that this property is built into the oscillatory feedback loop rather than appended to it. It seems plausible that clocks are adjusted and reset through adjustments in central clock components such as frq, and, by extension, per.

摘要

在两种模式生物——粗糙脉孢菌和果蝇中,通过遗传学方法鉴定生物钟组件已取得成功。在每种生物中,通过筛选影响生物钟的突变所鉴定出的基因(粗糙脉孢菌中的frq、果蝇中的per)随后被证明具有核心生物钟组件的特征:(1)每个基因中的突变可影响周期长度和温度补偿,这是昼夜节律系统的两个典型特征;(2)每个基因以昼夜节律的方式调节自身转录的时间;(3)就frq而言,持续升高的表达在释放到正常条件下时会设定生物钟的相位。然而,尽管存在明显的遗传和分子相似性,但这两个基因既不是分子同源物也不是时间同源物。两个基因的表达峰值时间不同,frq的表达在黎明后达到峰值,而per的表达在午夜附近达到峰值。此外,虽然来自组成型启动子的per表达可以挽救缺乏该基因的果蝇的节律性,但frq的组成型表达不能挽救粗糙脉孢菌frq缺失菌株的节律性,实际上在野生型菌株中表达时会导致无节律性。这些数据表明frq是和/或编码昼夜节律振荡器的一个状态变量。最近对frq的分子遗传学分析揭示了温度补偿的起源,并强烈表明这种特性是内置在振荡反馈回路中而不是附加在其上。通过调整诸如frq以及由此延伸的per等核心生物钟组件来调整和重置生物钟似乎是合理的。

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