International Journal of Molecular Sciences (Nov 2021)

Mutants of the <i>white</i> ABCG Transporter in <i>Drosophila melanogaster</i> Have Deficient Olfactory Learning and Cholesterol Homeostasis

  • Jennifer L. Myers,
  • Maria Porter,
  • Nicholas Narwold,
  • Krishna Bhat,
  • Brigitte Dauwalder,
  • Gregg Roman

DOI
https://doi.org/10.3390/ijms222312967
Journal volume & issue
Vol. 22, no. 23
p. 12967

Abstract

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Drosophila’s white gene encodes an ATP-binding cassette G-subfamily (ABCG) half-transporter. White is closely related to mammalian ABCG family members that function in cholesterol efflux. Mutants of white have several behavioral phenotypes that are independent of visual defects. This study characterizes a novel defect of white mutants in the acquisition of olfactory memory using the aversive olfactory conditioning paradigm. The w1118 mutants learned slower than wildtype controls, yet with additional training, they reached wildtype levels of performance. The w1118 learning phenotype is also found in the wapricot and wcoral alleles, is dominant, and is rescued by genomic white and mini-white transgenes. Reducing dietary cholesterol strongly impaired olfactory learning for wildtype controls, while w1118 mutants were resistant to this deficit. The w1118 mutants displayed higher levels of cholesterol and cholesterol esters than wildtype under this low-cholesterol diet. Increasing levels of serotonin, dopamine, or both in the white mutants significantly improved w1118 learning. However, serotonin levels were not lower in the heads of the w1118 mutants than in wildtype controls. There were also no significant differences found in synapse numbers within the w1118 brain. We propose that the w1118 learning defect may be due to inefficient biogenic amine signaling brought about by altered cholesterol homeostasis.

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