The Autophagy Inducer Spermidine Protects Against Metabolic Dysfunction During Overnutrition

Author:

Liao Chen-Yu1ORCID,Kummert Oona M P1,Bair Amanda M1,Alavi Nora1ORCID,Alavi Josef1,Miller Delana M1,Bagga Isha1,Schempf Anja M1,Hsu Yueh-Mei1,Woods Bruce D1,Brown Mayfield Stephen M1,Mitchell Angelina N1,Tannady Gabriella1,Talbot Aislinn R1,Dueck Aaron M1,Barrera Ovando Ricardo1,Parker Heather D1,Wang Junying1,Schoeneweis Jane K1,Kennedy Brian K12

Affiliation:

1. Buck Institute for Research on Aging, Novato, California, USA

2. Healthy Longevity Programme, Yong Loo Lin of Medicine, National University of Singapore, Singapore

Abstract

Abstract Autophagy, a process catabolizing intracellular components to maintain energy homeostasis, impacts aging and metabolism. Spermidine, a natural polyamine and autophagy activator, extends life span across a variety of species, including mice. In addition to protecting cardiac and liver tissue, spermidine also affects adipose tissue through unexplored mechanisms. Here, we examined spermidine in the links between autophagy and systemic metabolism. Consistently, daily injection of spermidine delivered even at late life is sufficient to cause a trend in life-span extension in wild-type mice. We further found that spermidine has minimal metabolic effects in young and old mice under normal nutrition. However, spermidine counteracts high-fat diet (HFD)-induced obesity by increasing lipolysis in visceral fat. Mechanistically, spermidine increases the hepatokine fibroblast growth factor 21 (FGF21) expression in liver without reducing food intake. Spermidine also modulates FGF21 in adipose tissues, elevating FGF21 expression in subcutaneous fat, but reducing it in visceral fat. Despite this, FGF21 is not required for spermidine action, since Fgf21−/− mice were still protected from HFD. Furthermore, the enhanced lipolysis by spermidine was also independent of autophagy in adipose tissue, given that adipose-specific autophagy-deficient (Beclin-1flox/+Fabp4-cre) mice remained spermidine-responsive under HFD. Our results suggest that the metabolic effects of spermidine occur through systemic changes in metabolism, involving multiple mechanistic pathways.

Funder

National Institute on Aging

Glenn/AFAR

Publisher

Oxford University Press (OUP)

Subject

Geriatrics and Gerontology,Aging

Reference50 articles.

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