Cell Reports
Volume 22, Issue 10, 6 March 2018, Pages 2550-2556
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Innate Immune Signaling in Drosophila Blocks Insulin Signaling by Uncoupling PI(3,4,5)P3 Production and Akt Activation

https://doi.org/10.1016/j.celrep.2018.02.033Get rights and content
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Highlights

  • Toll acts cell autonomously to induce insulin resistance in the Drosophila fat body

  • Fat body Toll signaling reduces growth and triglyceride storage without altering circulating Dilp2 levels

  • Toll signaling acts at or downstream of the kinase Pdk1 to reduce Akt phosphorylation

  • Mimicking Akt activation loop phosphorylation rescues Toll-dependent phenotypes

Summary

In obese adipose tissue, Toll-like receptor signaling in macrophages leads to insulin resistance in adipocytes. Similarly, Toll signaling in the Drosophila larval fat body blocks insulin-dependent growth and nutrient storage. We find that Toll acts cell autonomously to block growth but not PI(3,4,5)P3 production in fat body cells expressing constitutively active PI3K. Fat body Toll signaling blocks whole-animal growth in rictor mutants lacking TORC2 activity, but not in larvae lacking Pdk1. Phosphorylation of Akt on the Pdk1 site, Thr342, is significantly reduced by Toll signaling, and expression of mutant AktT342D rescues cell and animal growth, nutrient storage, and viability in animals with active Toll signaling. Altogether, these data show that innate immune signaling blocks insulin signaling at a more distal level than previously appreciated, and they suggest that manipulations affecting the Pdk1 arm of the pathway may have profound effects on insulin sensitivity in inflamed tissues.

Keywords

insulin resistance
innate immune signaling
inflammation
growth
Akt
Pdk1
Toll
Toll-like receptor
Drosophila

Cited by (0)

3

Present address: Internal Medicine Research Unit, Pfizer, Inc., Cambridge, MA 02139, USA

4

Lead Contact