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Publication : Multiomics assessment of dietary protein titration reveals altered hepatic glucose utilization.

First Author  MacArthur MR Year  2022
Journal  Cell Rep Volume  40
Issue  7 Pages  111187
PubMed ID  35977507 Mgi Jnum  J:330811
Mgi Id  MGI:7332647 Doi  10.1016/j.celrep.2022.111187
Citation  MacArthur MR, et al. (2022) Multiomics assessment of dietary protein titration reveals altered hepatic glucose utilization. Cell Rep 40(7):111187
abstractText  Dietary protein restriction (PR) has rapid effects on metabolism including improved glucose and lipid homeostasis, via multiple mechanisms. Here, we investigate responses of fecal microbiome, hepatic transcriptome, and hepatic metabolome to six diets with protein from 18% to 0% of energy in mice. PR alters fecal microbial composition, but metabolic effects are not transferable via fecal transplantation. Hepatic transcriptome and metabolome are significantly altered in diets with lower than 10% energy from protein. Changes upon PR correlate with calorie restriction but with a larger magnitude and specific changes in amino acid (AA) metabolism. PR increases steady-state aspartate, serine, and glutamate and decreases glucose and gluconeogenic intermediates. (13)C6 glucose and glycerol tracing reveal increased fractional enrichment in aspartate, serine, and glutamate. Changes remain intact in hepatic ATF4 knockout mice. Together, this demonstrates an ATF4-independent shift in gluconeogenic substrate utilization toward specific AAs, with compensation from glycerol to promote a protein-sparing response.
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