Hayley T. Schultz scite author profile

Background: miR-33 family members are well characterized regulators of cellular lipid levels in mammals. Previous studies have shown that overexpression of miR-33 in Drosophila melanogaster leads to elevated triacylglycerol (TAG) levels in certain contexts. Although loss of miR-33 in flies causes subtle defects in larval and adult ovaries, the effects of miR-33 deficiency on lipid metabolism and other phenotypes impacted by metabolic state have not yet been characterized. Results:We found that loss of miR-33 predisposes flies to elevated TAG levels, and we identified genes involved in TAG synthesis as direct targets of miR-33, including atpcl, midway, and Akt1. miR-33 mutants survived longer upon starvation but showed greater sensitivity to an oxidative stressor. We also found evidence that miR-33 is a negative regulator of cuticle pigmentation and that miR-33 mutants show a reduction in interfollicular stalk cells during oogenesis. Conclusion:Our data suggest that miR-33 is a conserved regulator of lipid homeostasis, and its targets are involved in both degradation and synthesis of fatty acids and TAG. The constellation of phenotypes involving tissues that are highly sensitive to metabolic state suggests that miR-33 serves to prevent extreme fluctuations in metabolically sensitive tissues.

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Genome-wide functional perturbation of human microsatellite repeats using engineered zinc finger transcription factors

Tak

Boulay

Lee

et al. 2022

Cell Genomics

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Hayley T. Schultz

Augmenting and directing long-range CRISPR-mediated activation in human cells

The microRNA miR‐33 is a pleiotropic regulator of metabolic and developmental processes in Drosophila melanogaster

Genome-wide functional perturbation of human microsatellite repeats using engineered zinc finger transcription factors

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