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Maternal diet amplifies the hepatic aging trajectory of Cidea in male mice and leads to the development of fatty liver
Author(s) -
Carr Sarah K.,
Chen JianHua,
Cooper Wendy N.,
Constância Miguel,
Yeo Giles S. H.,
Ozanne Susan E.
Publication year - 2014
Publication title -
the faseb journal
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.709
H-Index - 277
eISSN - 1530-6860
pISSN - 0892-6638
DOI - 10.1096/fj.13-242727
Subject(s) - offspring , biology , oxidative stress , endocrinology , lipid metabolism , senescence , in utero , medicine , gene expression , epigenetics , physiology , andrology , microbiology and biotechnology , gene , genetics , pregnancy , fetus
The importance of the early environment on long‐term heath and life span is well documented. However, the molecular mechanisms mediating these effects remain poorly understood. Male offspring from a maternal protein restriction model, in which animals are exposed to a low‐protein diet while in utero and then are cross‐fostered to normally fed dams, demonstrate low birth weight, catch‐up growth, and reduced life span (recuperated offspring). In the current study, we used microarray analysis to identify hepatic genes that changed with age. Cell death‐inducing DNA fragmentation factor, α subunit‐like effector A (Cidea), a transcriptional coactivator that has been implicated in lipid accumulation demonstrated one of the largest age‐associated increases in expression (200‐fold, P <0.001). This increase was exaggerated ~ 3‐fold in recuperated offspring. These demonstrated increased hepatic lipid accumulation, higher levels of transcription factors important in lipid regulation, and greater oxidative stress. In vitro analysis revealed that Cidea expression was regulated by oxidative stress and DNA methylation. These findings suggest that maternal diet modulates the age‐associated changes in Cidea expression through several mechanisms. This expression affects hepatic lipid metabolism in these animals and thus provides a mechanism by which maternal diet can contribute to the metabolic health and ultimately the life span of the offspring.—Carr, S. K., Chen, J.‐H., Cooper, W. N., Constância, M., Yeo, G. S. H., Ozanne, S. E. Maternal diet amplifies the hepatic ageing trajectory of Cidea in male mice and leads to the development of fatty liver. FASEB J . 28, 2191–2201 (2014). www.fasebj.org