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daf-28 encodes a C. elegans insulin superfamily member that is regulated by environmental cues and acts in the DAF-2 signaling pathway

机译:daf-28编码秀丽隐杆线虫胰岛素超家族成员该成员受环境信号调节并在DAF-2信号通路中起作用

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摘要

In Caenorhabditis elegans, the decision to enter a developmentally arrested dauer larval stage is triggered by a combination of signals from sensory neurons in response to environmental cues, which include a dauer pheromone. These sensory inputs are coupled to the parallel DAF-2/insulin receptor-like and DAF-7/TGFβ-like signaling pathways. Although sensory inputs have been shown to physiologically regulate DAF-7/TGFβ expression, no such regulation of insulin-like ligands in the DAF-2 pathway has been reported. We show here that daf-28 encodes an insulin-like protein, which when mutated causes dauer arrest and down-regulation of DAF-2/IR signaling. A daf-28∷GFP fusion gene is expressed in ASI and ASJ, two sensory neurons that regulate dauer arrest. daf-28∷GFP expression in ASI and ASJ is down-regulated under dauer-inducing conditions and in mutants of DAF-11/guanylyl cyclase, a predicted component of the dauer-pheromone-sensing pathway. Thus, daf-28 expression in sensory neurons is regulated by the environmental cues that normally trigger dauer arrest. Among the 38 C. elegans insulin genes, daf-28 is so far the only insulin mutant to affect dauer arrest. daf-28 was revealed from this functional redundancy by a dominant-negative allele that disrupts a probable proteolytic processing site required for insulin maturation. This DAF-28 mutant is likely to be poisonous to wild-type DAF-28 and other insulins.
机译:在秀丽隐杆线虫中,进入发育停滞的dauer幼虫阶段的决定是由来自感官神经元的信号组合响应环境提示而触发的,其中包括dauer信息素。这些感觉输入耦合到平行的DAF-2 /胰岛素受体样和DAF-7 /TGFβ样信号通路。尽管已经显示感觉输入在生理上调节DAF-7 /TGFβ的表达,但是尚未报道在DAF-2途径中胰岛素样配体的这种调节。我们在这里显示daf-28编码一种胰岛素样蛋白,该蛋白在突变时会导致dauer阻滞和DAF-2 / IR信号的下调。 daf-28∷GFP融合基因在ASI和ASJ中表达,这是两个调节dauer阻滞的感觉神经元。 daf-28∷GFP在dauer诱导条件下以及DAF-11 /鸟苷酸环化酶突变体中被下调,该突变体是dauer-信息素传感途径的预测成分。因此,感觉神经元中的daf-28表达受正常情况下触发dauer阻滞的环境提示的调节。在38个秀丽隐杆线虫胰岛素基因中,daf-28是迄今为止唯一影响dauer阻滞的胰岛素突变体。 daf-28通过显性阴性等位基因从此功能冗余中揭示出来,该等位基因破坏了胰岛素成熟所需的可能的蛋白水解加工位点。该DAF-28突变体可能对野生型DAF-28和其他胰岛素有毒。

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