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Hexokinase is a key regulator of energy metabolism and ROS activity in insect lifespan extension

机译:己糖激酶是昆虫寿命延长中能量代谢和ROS活性的关键调节剂

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摘要

Developmental arrest (diapause) is a ‘non-aging’ state that is similar to the Caenorhabditis elegans dauer stage and Drosophila lifespan extension. Diapause results in low metabolic activity and a profound extension of insect lifespan. Here, we cloned the Helicoverpa armigera Hexokinase (HK) gene, a gene that is critical for the developmental arrest of this species. HK expression and activity levels were significantly increased in nondiapause-destined pupae compared with those of diapause-destined pupae. Downregulation of HK activity reduced cell viability and delayed pupal development by reducing metabolic activity and increasing ROS activity, which suggests that HK is a key regulator of insect development. We then identified the transcription factors Har-CREB, -c-Myc, and -POU as specifically binding the Har-HK promoter and regulating its activity. Intriguingly, Har-POU and -c-Myc are specific transcription factors for HK expression, whereas Har-CREB is nonspecific. Furthermore, Har-POU and -c-Myc could respond to ecdysone, which is an upstream hormone. Therefore, low ecdysone levels in diapause-destined individuals lead to low Har-POU and -c-Myc expression levels, ultimately repressing Har-HK expression and inducing entry into diapause or lifespan extension.
机译:发育停滞(糖尿病)是一种“非衰老”状态,类似于秀丽隐杆线虫的阶段和果蝇的寿命延长。滞育导致新陈代谢活动降低,并大大延长了昆虫的寿命。在这里,我们克隆了棉铃虫Hexokinase(HK)基因,该基因对该物种的发育停滞至关重要。与以滞育为目的的up相比,非滞留性的的HK表达和活性水平显着增加。 HK活性的下调通过降低代谢活性和增加ROS活性而降低了细胞活力并延缓了幼虫的发育,这表明HK是昆虫发育的关键调节剂。然后,我们确定了转录因子Har-CREB,-c-Myc和-POU与Har-HK启动子特异性结合并调节其活性。有趣的是,Har-POU和-c-Myc是HK表达的特异性转录因子,而Har-CREB是非特异性的。此外,Har-POU和-c-Myc可以对蜕皮激素(一种上游激素)产生反应。因此,以滞育为目标的个体中的蜕皮激素水平低会导致Har-POU和-c-Myc表达水平低,最终抑制Har-HK表达并诱导进入滞育或延长寿命。

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