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Freeze–thaw Caenorhabditis elegans freeze–thaw stress response is regulated by the insulin/IGF-1 receptor daf-2

机译:冻融线虫秀丽隐杆线虫冻融应激反应受胰岛素/ IGF-1受体daf-2调节。

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Background Adaption to cold temperatures, especially those below freezing, is essential for animal survival in cold environments. Freezing is also used for many medical, scientific, and industrial purposes. Natural freezing survival in animals has been extensively studied. However, the underlying mechanisms remain unclear. Previous studies demonstrated that animals survive in extremely cold weather by avoiding freezing or controlling the rate of ice-crystal formation in their bodies, which indicates that freezing survival is a passive thermodynamic process. Results Here, we showed that genetic programming actively promotes freezing survival in Caenorhabditis elegans . We found that daf-2 , an insulin/IGF-1 receptor homologue, and loss-of-function enhanced survival during freeze–thaw stress, which required the transcription factor daf-16 /FOXO and age-independent target genes. In particular, the freeze–thaw resistance of daf-2 (rf) is highly allele-specific and has no correlation with lifespan, dauer formation, or hypoxia stress resistance. Conclusions Our results reveal a new function for daf-2 signaling, and, most importantly, demonstrate that genetic programming contributes to freezing survival.
机译:背景技术适应寒冷温度,尤其是低于冰点的温度,对于动物在寒冷环境中的生存至关重要。冷冻还用于许多医学,科学和工业目的。动物的自然冷冻存活已被广泛研究。但是,其潜在机制仍不清楚。先前的研究表明,动物可以通过避免冰冻或控制体内冰晶形成的速度来在极端寒冷的天气中生存,这表明冰冻生存是一个被动的热力学过程。结果在这里,我们表明遗传程序设计可以积极促进秀丽隐杆线虫的冷冻存活。我们发现,daf-2(一种胰岛素/ IGF-1受体的同系物)和功能丧失提高了冻融压力下的存活率,这需要转录因子daf-16 / FOXO和不依赖年龄的靶基因。特别是daf-2(rf)的抗冻融性是高度等位基因特异性的,与寿命,dauer形成或低氧胁迫抗性没有关系。结论我们的结果揭示了daf-2信号转导的新功能,最重要的是,证明了基因编程有助于冷冻存活。

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