Angptl3 regulates lipid metabolism in mice

R Koishi, Y Ando, M Ono, M Shimamura, H Yasumo… - Nature …, 2002 - nature.com
R Koishi, Y Ando, M Ono, M Shimamura, H Yasumo, T Fujiwara, H Horikoshi, H Furukawa
Nature genetics, 2002nature.com
The KK obese mouse is moderately obese and has abnormally high levels of plasma insulin
(hyperinsulinemia), glucose (hyperglycemia) and lipids (hyperlipidemia). In one strain
(KK/San), we observed abnormally low plasma lipid levels (hypolipidemia). This mutant
phenotype is inherited recessively as a mendelian trait. Here we report the mapping of the
hypolipidemia (hypl) locus to the middle of chromosome 4 and positional cloning of the
autosomal recessive mutation responsible for the hypolipidemia. The hypl locus encodes a …
Abstract
The KK obese mouse is moderately obese and has abnormally high levels of plasma insulin (hyperinsulinemia), glucose (hyperglycemia) and lipids (hyperlipidemia). In one strain (KK/San), we observed abnormally low plasma lipid levels (hypolipidemia). This mutant phenotype is inherited recessively as a mendelian trait. Here we report the mapping of the hypolipidemia (hypl) locus to the middle of chromosome 4 and positional cloning of the autosomal recessive mutation responsible for the hypolipidemia. The hypl locus encodes a unique angiopoietin-like lipoprotein modulator, which we named Allm1. It is identical to angiopoietin-like protein 3, encoded by Angptl3, and has a highly conserved counterpart in humans. Overexpression of Angptl3 or intravenous injection of the purified protein in KK/San mice elicited an increase in circulating plasma lipid levels. This increase was also observed in C57BL/6J normal mice. Taken together, these data suggest that Angptl3 regulates lipid metabolism in animals.
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