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SREBP-2-deficient and hypomorphic mice reveal roles for SREBP-2 in embryonic development and SREBP-1c expression

Authors :
Laurent Vergnes
Timothy F. Osborne
Robert Chin
Loren G. Fong
Thomas Q. de Aguiar Vallim
Stephen G. Young
Karen Reue
Source :
Journal of lipid research, vol 57, iss 3, Journal of Lipid Research, Vol 57, Iss 3, Pp 410-421 (2016)
Publication Year :
2016
Publisher :
eScholarship, University of California, 2016.

Abstract

Cholesterol and fatty acid biosynthesis are regulated by the sterol regulatory element-binding proteins (SREBPs), encoded by Srebf1 and Srebf2. We generated mice that were either deficient or hypomorphic for SREBP-2. SREBP-2 deficiency generally caused death during embryonic development. Analyses of Srebf2(-/-) embryos revealed a requirement for SREBP-2 in limb development and expression of morphogenic genes. We encountered only one viable Srebf2(-/-) mouse, which displayed alopecia, attenuated growth, and reduced adipose tissue stores. Hypomorphic SREBP-2 mice (expressing low levels of SREBP-2) survived development, but the female mice exhibited reduced body weight and died between 8 and 12 weeks of age. Male hypomorphic mice were viable but had reduced cholesterol stores in the liver and lower expression of SREBP target genes. Reduced SREBP-2 expression affected SREBP-1 isoforms in a tissue-specific manner. In the liver, reduced SREBP-2 expression nearly abolished Srebf1c transcripts and reduced Srebf1a mRNA levels. In contrast, adipose tissue displayed normal expression of SREBP target genes, likely due to a compensatory increase in Srebf1a expression. Our results establish that SREBP-2 is critical for survival and limb patterning during development. Reduced expression of SREBP-2 from the hypomorphic allele leads to early death in females and reduced cholesterol content in the liver, but not in adipose tissue.

Details

Database :
OpenAIRE
Journal :
Journal of lipid research, vol 57, iss 3, Journal of Lipid Research, Vol 57, Iss 3, Pp 410-421 (2016)
Accession number :
edsair.doi.dedup.....d2661d333899e6d9cb818c5039cd0a67