4.8 Article

A nutrient-responsive hormonal circuit mediates an inter-tissue program regulating metabolic homeostasis in adult Drosophila

Journal

NATURE COMMUNICATIONS
Volume 12, Issue 1, Pages -

Publisher

NATURE PORTFOLIO
DOI: 10.1038/s41467-021-25445-2

Keywords

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Funding

  1. Villum Foundation [15365]
  2. Danish Council for Independent Research Natural Sciences [9064-00009B]
  3. UKRI BBSRC [BB/P008097/1]
  4. Novo Nordisk Foundation [16OC0021270]
  5. United Kingdom Medical Research Council [MC_ UU_12014/8]
  6. BBSRC [BB/P008097/1] Funding Source: UKRI
  7. MRC [MC_UU_12014/8] Funding Source: UKRI

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Neurosecretory cells in Drosophila release Capa hormones in response to nutrient levels, activating the Capa receptor in peripheral tissues to regulate energy homeostasis. Disruption of Capa/CapaR signaling leads to intestinal hypomotility and impaired nutrient absorption, depleting internal nutrient stores. Additionally, Capa/CapaR inhibits the release of a hormone that mobilizes energy from adipose tissue to prevent harmful hyperglycemia.
Animals maintain metabolic homeostasis by modulating the activity of specialized organs that adjust internal metabolism to external conditions. However, the hormonal signals coordinating these functions are incompletely characterized. Here we show that six neurosecretory cells in the Drosophila central nervous system respond to circulating nutrient levels by releasing Capa hormones, homologs of mammalian neuromedin U, which activate the Capa receptor (CapaR) in peripheral tissues to control energy homeostasis. Loss of Capa/CapaR signaling causes intestinal hypomotility and impaired nutrient absorption, which gradually deplete internal nutrient stores and reduce organismal lifespan. Conversely, increased Capa/CapaR activity increases fluid and waste excretion. Furthermore, Capa/CapaR inhibits the release of glucagon-like adipokinetic hormone from the corpora cardiaca, which restricts energy mobilization from adipose tissue to avoid harmful hyperglycemia. Our results suggest that the Capa/CapaR circuit occupies a central node in a homeostatic program that facilitates the digestion and absorption of nutrients and regulates systemic energy balance.

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