An excreted small molecule promotes C. elegans reproductive development and aging

生物 秀丽隐杆线虫 雌雄同体 滞育 长寿 交配 激素 核受体 细胞生物学 遗传学 幼虫 内分泌学 动物 生态学 基因 转录因子
作者
Andreas H. Ludewig,Alexander B. Artyukhin,Erin Z. Aprison,Pedro R. Rodrigues,Dania Camila Pulido,Russell N. Burkhardt,Oishika Panda,Ying K. Zhang,Pooja Gudibanda,Ilya Ruvinsky,Frank C. Schroeder
出处
期刊:Nature Chemical Biology [Springer Nature]
卷期号:15 (8): 838-845 被引量:55
标识
DOI:10.1038/s41589-019-0321-7
摘要

Excreted small-molecule signals can bias developmental trajectories and physiology in diverse animal species. However, the chemical identity of these signals remains largely obscure. Here we report identification of an unusual N-acylated glutamine derivative, nacq#1, that accelerates reproductive development and shortens lifespan in Caenorhabditis elegans. Produced predominantly by C. elegans males, nacq#1 hastens onset of sexual maturity in hermaphrodites by promoting exit from the larval dauer diapause and by accelerating late larval development. Even at picomolar concentrations, nacq#1 shortens hermaphrodite lifespan, suggesting a trade-off between reproductive investment and longevity. Acceleration of development by nacq#1 requires chemosensation and is dependent on three homologs of vertebrate steroid hormone receptors. Unlike ascaroside pheromones, which are restricted to nematodes, fatty acylated amino acid derivatives similar to nacq#1 have been reported from humans and invertebrates, suggesting that related compounds may serve signaling functions throughout metazoa. Male C. elegans excrete an N-acylated glutamine that acts via evolutionarily conserved nuclear hormone receptor and chemosensory pathways to counteract dauer diapause and accelerate sexual maturation of hermaphrodites, at the cost of shortening hermaphrodite lifespan.
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