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Regular Research Articles
2 Results
- Research ArticleOpen Access
Sar1b mutant mice recapitulate gastrointestinal abnormalities associated with chylomicron retention disease
Journal of Lipid ResearchVol. 62100085Published online: May 5, 2021- Nickolas Auclair
- Alain T. Sané
- Lena Ahmarani
- Nathalie Patey
- Jean-François Beaulieu
- Noel Peretti
- and others
Cited in Scopus: 0Chylomicron retention disease (CRD) is an autosomal recessive disorder associated with biallelic Sar1b mutations leading to defects in intracellular chylomicron (CM) trafficking and secretion. To date, a direct cause-effect relationship between CRD and Sar1b mutation has not been established, but genetically modified animal models provide an opportunity to elucidate unrecognized aspects of these mutations. To examine the physiological role and molecular mechanisms of Sar1b function, we generated mice expressing either a targeted deletion or mutation of human Sar1b using the CRISPR-Cas9 system. - Research ArticleOpen Access
Hepatic deletion of Mboat7 (LPIAT1) causes activation of SREBP-1c and fatty liver
Journal of Lipid ResearchVol. 62100031Published online: February 5, 2021- Mingfeng Xia
- Preethi Chandrasekaran
- Shunxing Rong
- Xiaorong Fu
- Matthew A. Mitsche
Cited in Scopus: 0Genetic variants that increase the risk of fatty liver disease and cirrhosis have recently been identified in the proximity of membrane-bound O-acyltransferase domain-containing 7 (MBOAT7). To elucidate the link between these variants and fatty liver disease, we characterized Mboat7 liver-specific KO mice (Mboat7 LSKO). Chow-fed Mboat7 LSKO mice developed fatty livers and associated liver injury. Lipidomic analysis of liver using MS revealed a pronounced reduction in 20-carbon PUFA content in phosphatidylinositols (PIs) but not in other phospholipids.