Identification of circadian clock modulators from existing drugs.
T Katherine TamaiYusuke NakaneWataru OtaAkane KobayashiMasateru IshiguroNaoya KadofusaKeisuke IkegamiKazuhiro YagitaYasufumi ShigeyoshiMasaki SudoTaeko Nishiwaki-OhkawaAyato SatoTakashi YoshimuraPublished in: EMBO molecular medicine (2019)
Chronic circadian disruption due to shift work or frequent travel across time zones leads to jet-lag and an increased risk of diabetes, cardiovascular disease, and cancer. The development of new pharmaceuticals to treat circadian disorders, however, is costly and hugely time-consuming. We therefore performed a high-throughput chemical screen of existing drugs for circadian clock modulators in human U2OS cells, with the aim of repurposing known bioactive compounds. Approximately 5% of the drugs screened altered circadian period, including the period-shortening compound dehydroepiandrosterone (DHEA; also known as prasterone). DHEA is one of the most abundant circulating steroid hormones in humans and is available as a dietary supplement in the USA Dietary administration of DHEA to mice shortened free-running circadian period and accelerated re-entrainment to advanced light-dark (LD) cycles, thereby reducing jet-lag. Our drug screen also revealed the involvement of tyrosine kinases, ABL1 and ABL2, and the BCR serine/threonine kinase in regulating circadian period. Thus, drug repurposing is a useful approach to identify new circadian clock modulators and potential therapies for circadian disorders.
Keyphrases
- high throughput
- cardiovascular disease
- tyrosine kinase
- small molecule
- type diabetes
- induced apoptosis
- high frequency
- drug induced
- protein kinase
- single cell
- emergency department
- acute lymphoblastic leukemia
- oxidative stress
- squamous cell carcinoma
- papillary thyroid
- high intensity
- skeletal muscle
- endoplasmic reticulum stress
- cardiovascular risk factors