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Dietary restriction induces a sexually dimorphic type I interferon response in mice with gene-environment interactions

Dylan Harney, Michelle Cielesh, G. Evan Roberts, Isabelle K. Vila, Barney Viengkhou, Markus J. Hofer, Nadine Laguette, Mark Larance

2023Cell Reports14 citationsDOIOpen Access PDF

Abstract

Intermittent fasting (IF) is an established intervention to treat the growing obesity epidemic. However, the interaction between dietary interventions and sex remains a significant knowledge gap. In this study, we use unbiased proteome analysis to identify diet-sex interactions. We report sexual dimorphism in response to intermittent fasting within lipid and cholesterol metabolism and, unexpectedly, in type I interferon signaling, which was strongly induced in females. We verify that secretion of type I interferon is required for the IF response in females. Gonadectomy differentially alters the every-other-day fasting (EODF) response and demonstrates that sex hormone signaling can either suppress or enhance the interferon response to IF. IF fails to potentiate a stronger innate immune response when IF-treated animals were challenged with a viral mimetic. Lastly, the IF response changes with genotype and environment. These data reveal an interesting interaction between diet, sex, and the innate immune system.

Topics & Concepts

InterferonBiologySexual dimorphismInnate immune systemImmune systemInterferon type IGenotypeEndocrinologyObesityGeneInternal medicineImmunologyGeneticsMedicineDietary Effects on HealthCancer-related molecular mechanisms researchCircadian rhythm and melatonin