| Literature DB >> 35108511 |
Cara L Green1, Heidi H Pak2, Nicole E Richardson3, Victoria Flores2, Deyang Yu4, Jay L Tomasiewicz5, Sabrina N Dumas1, Katherine Kredell1, Jesse W Fan1, Charlie Kirsh6, Krittisak Chaiyakul7, Michaela E Murphy2, Reji Babygirija8, Gregory A Barrett-Wilt9, Joshua Rabinowitz10, Irene M Ong11, Cholsoon Jang12, Judith Simcox13, Dudley W Lamming14.
Abstract
Low-protein diets promote metabolic health in humans and rodents. Despite evidence that sex and genetic background are key factors in the response to diet, most protein intake studies examine only a single strain and sex of mice. Using multiple strains and both sexes of mice, we find that improvements in metabolic health in response to reduced dietary protein strongly depend on sex and strain. While some phenotypes were conserved across strains and sexes, including increased glucose tolerance and energy expenditure, we observed high variability in adiposity, insulin sensitivity, and circulating hormones. Using a multi-omics approach, we identified mega-clusters of differentially expressed hepatic genes, metabolites, and lipids associated with each phenotype, providing molecular insight into the differential response to protein restriction. Our results highlight the importance of sex and genetic background in the response to dietary protein level, and the potential importance of a personalized medicine approach to dietary interventions. Published by Elsevier Inc.Entities:
Keywords: FGF21; UM-HET3; genetic variation; liver; metabolic health; multi-omics; precision dietetics; protein restriction; sexual dimorphism
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Year: 2022 PMID: 35108511 PMCID: PMC8865085 DOI: 10.1016/j.cmet.2021.12.018
Source DB: PubMed Journal: Cell Metab ISSN: 1550-4131 Impact factor: 27.287