Sestrin mediates detection of and adaptation to low-leucine diets in Drosophila.
Xin GuPatrick JouandinPranav V LalgudiRich BinariMax L ValensteinMichael A ReidAnnamarie E AllenNolan KamitakiJason W LocasaleNorbert PerrimonDavid M SabatiniPublished in: Nature (2022)
Mechanistic target of rapamycin complex 1 (mTORC1) regulates cell growth and metabolism in response to multiple nutrients, including the essential amino acid leucine 1 . Recent work in cultured mammalian cells established the Sestrins as leucine-binding proteins that inhibit mTORC1 signalling during leucine deprivation 2,3 , but their role in the organismal response to dietary leucine remains elusive. Here we find that Sestrin-null flies (Sesn -/- ) fail to inhibit mTORC1 or activate autophagy after acute leucine starvation and have impaired development and a shortened lifespan on a low-leucine diet. Knock-in flies expressing a leucine-binding-deficient Sestrin mutant (Sesn L431E ) have reduced, leucine-insensitive mTORC1 activity. Notably, we find that flies can discriminate between food with or without leucine, and preferentially feed and lay progeny on leucine-containing food. This preference depends on Sestrin and its capacity to bind leucine. Leucine regulates mTORC1 activity in glial cells, and knockdown of Sesn in these cells reduces the ability of flies to detect leucine-free food. Thus, nutrient sensing by mTORC1 is necessary for flies not only to adapt to, but also to detect, a diet deficient in an essential nutrient.