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SREBP1c-CRY1 signalling represses hepatic glucose production by promoting FOXO1 degradation during refeeding

The clock protein Cry regulates hepatic glucose metabolism. Here the authors show that SREBP1c, activated by insulin signalling after feeding, directly regulates Cry transcription at specific circadian time points, and that Cry represses hepatic glucose production by promoting proteasomal degradation of Foxo1.

Hagoon Jang
Gha Young Lee
Jae Bum Kim
ResearchOpen Access14 Jul 2016
Nature Communications

Volume: 7, P: 1-14
Spatiotemporal contact between peroxisomes and lipid droplets regulates fasting-induced lipolysis via PEX5

Lipid droplets are organelles that regulate lipid metabolism but if organellar contacts play a role during lipolysis is unclear. Here, the authors show that peroxisomes and peroxisomal protein PEX5 play pivotal roles in the spatial and temporal regulation of fasting-induced lipolysis by translocating ATGL onto lipid droplets

Jinuk Kong
Yul Ji
Jae Bum Kim
ResearchOpen Access29 Jan 2020
Nature Communications

Volume: 11, P: 1-16
Fludarabine increases nuclease-free AAV- and CRISPR/Cas9-mediated homologous recombination in mice

Fludarabine-induced DNA damage pathways enhance the in vivo efficiency of homologous recombination-based gene editing.

Shinnosuke Tsuji
Calvin J. Stephens
Mark A. Kay
Research07 Apr 2022
Nature Biotechnology

Volume: 40, P: 1285-1294

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