PLoS Genetics (Mar 2015)

Methyl farnesoate plays a dual role in regulating Drosophila metamorphosis.

  • Di Wen,
  • Crisalejandra Rivera-Perez,
  • Mohamed Abdou,
  • Qiangqiang Jia,
  • Qianyu He,
  • Xi Liu,
  • Ola Zyaan,
  • Jingjing Xu,
  • William G Bendena,
  • Stephen S Tobe,
  • Fernando G Noriega,
  • Subba R Palli,
  • Jian Wang,
  • Sheng Li

DOI
https://doi.org/10.1371/journal.pgen.1005038
Journal volume & issue
Vol. 11, no. 3
p. e1005038

Abstract

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Corpus allatum (CA) ablation results in juvenile hormone (JH) deficiency and pupal lethality in Drosophila. The fly CA produces and releases three sesquiterpenoid hormones: JH III bisepoxide (JHB3), JH III, and methyl farnesoate (MF). In the whole body extracts, MF is the most abundant sesquiterpenoid, followed by JHB3 and JH III. Knockout of JH acid methyl transferase (jhamt) did not result in lethality; it decreased biosynthesis of JHB3, but MF biosynthesis was not affected. RNAi-mediated reduction of 3-hydroxy-3-methylglutaryl CoA reductase (hmgcr) expression in the CA decreased biosynthesis and titers of the three sesquiterpenoids, resulting in partial lethality. Reducing hmgcr expression in the CA of the jhamt mutant further decreased MF titer to a very low level, and caused complete lethality. JH III, JHB3, and MF function through Met and Gce, the two JH receptors, and induce expression of Kr-h1, a JH primary-response gene. As well, a portion of MF is converted to JHB3 in the hemolymph or peripheral tissues. Topical application of JHB3, JH III, or MF precluded lethality in JH-deficient animals, but not in the Met gce double mutant. Taken together, these experiments show that MF is produced by the larval CA and released into the hemolymph, from where it exerts its anti-metamorphic effects indirectly after conversion to JHB3, as well as acting as a hormone itself through the two JH receptors, Met and Gce.