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穿梭飞船基因是果蝇中一个与神经元发育有关的基因,其胚胎期表达与成虫寿命相关。

Embryonic expression of shuttle craft, a Drosophila gene involved in neuron development, is associated with adult lifespan.

作者信息

Roshina Natalia V, Symonenko Alexander V, Krementsova Anna V, Trostnikov Mikhail V, Pasyukova Elena G

机构信息

Institute of Molecular Genetics of Russian Academy of Sciences, Moscow, 123182, Russia.

出版信息

Aging (Albany NY). 2014 Dec;6(12):1076-93. doi: 10.18632/aging.100712.

Abstract

Despite the progress in aging research that highlights the role of the nervous system in longevity, whether genes that control development and consequently structure of the nervous system affect lifespan is unclear. We demonstrated that a mutation inshuttle craft, a gene involved in the nervous system development, increased the lifespan of unmated females and decreased the lifespan of mated females, without affecting males. Precise reversions of the mutation lead to the restoration of the lifespan specific to control females. In mutant unmated females, increased lifespan was associated with elevated locomotion at older ages, indicating slowed aging. In mutant mated females, reproduction was decreased compared to controls, indicating a lack of tradeoff between this trait and lifespan. No differences in shuttle craft transcription were observed between whole bodies, ovaries, and brains of mutant and control females of different ages, either unmated or mated. The amount of shuttle craft transcript appeared to be substantially decreased in mutant embryos. Our results demonstrated that a gene that regulates development of the nervous system might also influence longevity, and thus expanded the spectrum of genes involved in lifespan control. We hypothesize that this "carry-over" effect might be the result of transcription regulation in embryos.

摘要

尽管衰老研究取得了进展,突出了神经系统在长寿中的作用,但控制神经系统发育进而结构的基因是否影响寿命仍不清楚。我们证明,参与神经系统发育的基因“穿梭飞船”发生突变后,未交配雌性的寿命延长,而交配雌性的寿命缩短,对雄性没有影响。该突变的精确回复导致恢复到对照雌性特有的寿命。在突变的未交配雌性中,寿命延长与老年时运动能力增强有关,表明衰老减缓。在突变的交配雌性中,与对照相比繁殖能力下降,表明该性状与寿命之间不存在权衡。在不同年龄的未交配或交配的突变雌性和对照雌性的全身、卵巢和大脑之间,未观察到“穿梭飞船”转录的差异。在突变胚胎中,“穿梭飞船”转录本的量似乎大幅减少。我们的结果表明,一个调节神经系统发育的基因可能也会影响寿命,从而扩大了参与寿命控制的基因谱。我们推测这种“遗留”效应可能是胚胎中转录调控的结果。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2526/4298367/ce61a9f3d282/aging-06-1076-g001.jpg

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