4.5 Article

Insulin-like peptide genes in honey bee fat body respond differently to manipulation of social behavioral physiology

Journal

JOURNAL OF EXPERIMENTAL BIOLOGY
Volume 214, Issue 9, Pages 1488-1497

Publisher

COMPANY OF BIOLOGISTS LTD
DOI: 10.1242/jeb.050393

Keywords

peripheral insulin-like signaling; vitellogenin; division of labor; nutrition; RNA-interference

Categories

Funding

  1. Norwegian Research Council [180504, 185306, 191699]
  2. PEW Foundation
  3. National Institute of Aging (NIA) [P01 AG22500]
  4. CNPq [305378/2007-4]
  5. National Science Foundation [0910330]
  6. Arizona State University-Smithsonian Tropical Research Institute post-doctoral award
  7. Division Of Integrative Organismal Systems
  8. Direct For Biological Sciences [0910330] Funding Source: National Science Foundation

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Nutrient sensitive insulin-like peptides (ILPs) have profound effects on invertebrate metabolism, nutrient storage, fertility and aging. Many insects transcribe ILPs in specialized neurosecretory cells at changing levels correlated with life history. However, the major site of insect metabolism and nutrient storage is not the brain, but rather the fat body, where functions of ILP expression are rarely studied and poorly understood. Fat body is analogous to mammalian liver and adipose tissue, with nutrient stores that often correlate with behavior. We used the honey bee (Apis mellifera), an insect with complex behavior, to test whether ILP genes in fat body respond to experimentally induced changes of behavioral physiology. Honey bee fat body influences endocrine state and behavior by secreting the yolk protein precursor vitellogenin (Vg), which suppresses lipophilic juvenile hormone and social foraging behavior. In a two-factorial experiment, we used RNA interference (RNAi)-mediated vg gene knockdown and amino acid nutrient enrichment of hemolymph (blood) to perturb this regulatory module. We document factor-specific changes in fat body ilp1 and ilp2 mRNA, the bee's ILP-encoding genes, and confirm that our protocol affects social behavior. We show that ilp1 and ilp2 are regulated independently and differently and diverge in their specific expression-localization between fat body oenocyte and trophocyte cells. Insect ilp functions may be better understood by broadening research to account for expression in fat body and not only brain.

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