Juvenile hormone suppresses the FoxO-takeout axis to shorten longevity in male silkworm

保幼激素 生物 长寿 甲基戊烯 尿管体 内分泌学 变形 内科学 基因敲除 转录因子 信号转导 基因 细胞生物学 激素 遗传学 幼虫 生态学 医学
作者
Zhiquan Li,Jiangbo Song,Guihua Jiang,Yunzhu Shang,Yu Jiang,Jianfei Zhang,Xiao Li,Min Chen,Dongmei Tang,Xiaoling Tong,Fangyin Dai
出处
期刊:Pesticide Biochemistry and Physiology [Elsevier BV]
卷期号:192: 105388-105388 被引量:2
标识
DOI:10.1016/j.pestbp.2023.105388
摘要

Juvenile hormone (JH) plays a crucial endocrine regulatory role in insect metamorphosis, reproduction, and longevity in multiple organisms, such as flies, honeybees, and migratory monarch butterflies. However, the molecular mechanism of JH affecting longevity remains largely unknown. In this study, we showed that JH III and its analog methoprene shortened the survival days significantly in the adulthood of male silkworm. At the same time, the allatostatin, a neuropeptide that inhibits the secretion of JH by the corpora allata, could extend the survival days dramatically after adult eclosion in male silkmoth. Interestingly, a central pro-longevity FoxO transcription factor was reduced upon JH stimulation in silkworm individuals and BmN-SWU1 cells. Furthermore, the analysis of the upstream sequence of the FoxO gene identified a JH response element which suggested that FoxO might be regulated as a target of JH. Surprisingly, we identified a Bmtakeout (BmTO) gene that encodes a JH-binding protein and contains a FoxO response element. As expected, FoxO overexpression and knockdown up- and down-regulated the expression of BmTO respectively, indicating that BmTO functions as a FoxO target. BmTO overexpression could release the inhibitory effect of JH on the BmFoxO gene by reducing JH bioavailability to block its signal transduction. Collectively, these results may provide insights into the mechanism of the JH-FoxO-TO axis in aging research and pest control.
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