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Publication : Disruption of the circadian clock drives <i>Apc</i> loss of heterozygosity to accelerate colorectal cancer.

First Author  Chun SK Year  2022
Journal  Sci Adv Volume  8
Issue  32 Pages  eabo2389
PubMed ID  35947664 Mgi Jnum  J:327420
Mgi Id  MGI:7332342 Doi  10.1126/sciadv.abo2389
Citation  Chun SK, et al. (2022) Disruption of the circadian clock drives Apc loss of heterozygosity to accelerate colorectal cancer. Sci Adv 8(32):eabo2389
abstractText  An alarming rise in young onset colorectal cancer (CRC) has been reported; however, the underlying molecular mechanism remains undefined. Suspected risk factors of young onset CRC include environmental aspects, such as lifestyle and dietary factors, which are known to affect the circadian clock. We find that both genetic disruption and environmental disruption of the circadian clock accelerate Apc-driven CRC pathogenesis in vivo. Using an intestinal organoid model, we demonstrate that clock disruption promotes transformation by driving Apc loss of heterozygosity, which hyperactivates Wnt signaling. This up-regulates c-Myc, a known Wnt target, which drives heightened glycolytic metabolism. Using patient-derived organoids, we show that circadian rhythms are lost in human tumors. Last, we identify that variance between core clock and Wnt pathway genes significantly predicts the survival of patients with CRC. Overall, our findings demonstrate a previously unidentified mechanistic link between clock disruption and CRC, which has important implications for young onset cancer prevention.
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