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Reduced sleep in Drosophila shaker mutants

机译:果蝇振动筛突变体的睡眠减少

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Most of us sleep 7-8 h per night, and if we are deprived of sleep our performance suffers greatly; however, a few do well with just 3-4 h of sleep-a trait that seems to run in families. Determining which genes underlie this phenotype could shed light on the mechanisms and functions of sleep. To do so, we performed mutagenesis in Drosophila melanogaster, because flies also sleep for many hours and, when sleep deprived, show sleep rebound and performance impairments. By screening 9,000 mutant lines, we found minisleep (mns), a line that sleeps for one-third of the wild-type amount. We show that mns flies perform normally in a number of tasks, have preserved sleep homeostasis, but are not impaired by sleep deprivation. We then show that mns flies carry a point mutation in a conserved domain of the Shaker gene. Moreover, after crossing out genetic modifiers accumulated over many generations, other Shaker alleles also become short sleepers and fail to complement the mns phenotype. Finally, we show that short-sleeping Shaker flies have a reduced lifespan. Shaker, which encodes a voltage-dependent potassium channel controlling membrane repolarization and transmitter release, may thus regulate sleep need or efficiency.
机译:我们大多数人每晚睡眠7-8小时,如果我们缺乏睡眠,我们的表现会受到很大影响;但是,只有3-4小时的睡眠能很好地完成这一工作,这一特征似乎在家庭中普遍存在。确定哪些基因是该表型的基础,可以阐明睡眠的机制和功能。为此,我们在果蝇中进行了诱变,因为果蝇也睡了许多小时,并且当睡眠不足时,会表现出睡眠反弹和性能受损。通过筛选9,000个突变体系,我们发现了微型休眠(mns),该系休眠的数量为野生型数量的三分之一。我们显示,mns苍蝇在许多任务中都能正常执行,可以保持睡眠稳态,但不会因睡眠不足而受到损害。然后,我们显示mns蝇在Shaker基因的保守域中携带点突变。此外,在消除了多代积累的遗传修饰因子后,其他振动筛等位基因也变成了卧铺者,无法补充mns表型。最后,我们证明了摇摇欲坠的苍蝇的寿命缩短了。摇床编码的电压依赖性钾离子通道控制着膜的复极化和递质释放,因此可以调节睡眠需求或效率。

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