JhI-21 plays a role in Drosophila insulin-like peptide release from larval IPCs via leucine transport.
Anna B ZieglerGérard ManièreYael GrosjeanPublished in: Scientific reports (2018)
Insulin is present all across the animal kingdom. Its proper release after feeding is of extraordinary importance for nutrient uptake, regulation of metabolism, and growth. We used Drosophila melanogaster to shed light on the processes linking dietary leucine intake to insulin secretion. The Drosophila genome encodes 8 insulin-like peptides ("Dilps"). Of these, Dilp2 is secreted after the ingestion of a leucine-containing diet. We previously demonstrated that Minidiscs, related to mammalian system-L transporters, acts as a leucine sensor within the Dilp2-secreting insulin-producing cells ("IPCs") of the brain. Here, we show that a second leucine transporter, JhI-21, of the same family is additionally necessary for proper leucine sensing in the IPCs. Using calcium imaging and ex-vivo cultured brains we show that knockdown of JhI-21 in IPCs causes malfunction of these cells: they are no longer able to sense dietary leucine or to release Dilp2 in a leucine dependent manner. JhI-21 knockdown in IPCs further causes systemic metabolic defects including defective sugar uptake and altered growth. Finally, we showed that JhI-21 and Minidiscs have no cumulative effect on Dilp2 release. Since system-L transporters are expressed by mammalian β-cells our results could help to better understand the role of these proteins in insulin signaling.
Keyphrases
- type diabetes
- drosophila melanogaster
- induced apoptosis
- glycemic control
- cell cycle arrest
- signaling pathway
- gene expression
- body mass index
- multiple sclerosis
- oxidative stress
- endothelial cells
- adipose tissue
- skeletal muscle
- cell proliferation
- photodynamic therapy
- blood brain barrier
- brain injury
- weight gain
- genome wide