Steroids as central regulators of organismal development and lifespan

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Abstract

Larvae of the nematode Caenorhabditis elegans must choose between reproductive development and dauer diapause. This decision is based on sensing of environmental inputs and dauer pheromone, a small molecule signal that serves to monitor population density. These signals are integrated via conserved neuroendocrine pathways that converge on steroidal ligands of the nuclear receptor DAF-12, a homolog of the mammalian vitamin D receptor and liver X receptor. DAF-12 acts as the main switch between gene expression programs that drive either reproductive development or dauer entry. Extensive studies in the past two decades demonstrated that biosynthesis of two bile acid-like DAF-12 ligands, named dafachronic acids (DA), controls developmental fate. In this issue of PLoS Biology, Wollam et al. showed that a conserved steroid-modifying enzyme, DHS-16, introduces a key feature in the structures of the DAF-12 ligands, closing a major gap in the DA biosynthesis pathway. The emerging picture of DA biosynthesis in C. elegans enables us to address a key question in the field: how are complex environmental signals integrated to enforce binary, organism-wide decisions on developmental fate? Schaedel et al. demonstrated that pheromone and DA serve as competing signals, and that a positive feedback loop based on regulation of DA biosynthesis ensures organism-wide commitment to reproductive development. Considering that many components of DA signaling are highly conserved, ongoing studies in C. elegans may reveal new aspects of bile acid function and lifespan regulation in mammals. © 2012 Lee, Schroeder.

Figures

  • Figure 1. Dafachronic acid biosynthesis controls the decision between dauer and reproductive development. Insulin signaling and TGF-b signaling promote DA biosynthesis, driving development to reproductive adults, whereas dauer pheromone (ascarosides) abolish DA biosynthesis, resulting in unliganded DAF-12 and dauer formation. doi:10.1371/journal.pbio.1001307.g001
  • Figure 2. Dafachronic acid feedback directs organism-wide commitment to specific developmental fates. (A) Under favorable conditions, XXX-produced DA is amplified via daf-9 expression in hypodermal cells (green). (B) Under marginal conditions, increased hypodermal daf9 expression maintains sufficient DA levels to prevent intermediate phenotypes. (C) Under unfavorable conditions, low dafachronic acid production in the XXX cells is insufficient to turn on hypodermal DA production. The unliganded DAF-12 then recruits the corepressor DIN-1, promoting dauer development. doi:10.1371/journal.pbio.1001307.g002

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CITATION STYLE

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Lee, S. S., & Schroeder, F. C. (2012). Steroids as central regulators of organismal development and lifespan. PLoS Biology, 10(4). https://doi.org/10.1371/journal.pbio.1001307

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