Exome Sequencing,<i>ANGPTL3</i>Mutations, and Familial Combined Hypolipidemia

Kiran Musunuru; James P. Pirruccello; Ron Do; Gina M. Peloso; Candace Guiducci; Carrie Sougnez; Kiran Garimella; Sheila Fisher; Justin Abreu; Andrew J. Barry; Tim Fennell; Eric Banks; Lauren Ambrogio; Kristian Cibulskis; Andrew Kernytsky; Elena González; Nicholas Rudzicz; James C. Engert; Mark A. DePristo; Mark J. Daly; Jonathan C. Cohen; Helen H. Hobbs; David Altshuler; Gustav Schonfeld; Stacey Gabriel; Pin Yue; Sekar Kathiresan

doi:10.1056/nejmoa1002926

Exome Sequencing,<i>ANGPTL3</i>Mutations, and Familial Combined Hypolipidemia

Kiran Musunuru(Broad Institute), James P. Pirruccello(Broad Institute), Ron Do(Broad Institute), Gina M. Peloso(Boston University), Candace Guiducci(Broad Institute), Carrie Sougnez(Broad Institute), Kiran Garimella(Broad Institute), Sheila Fisher(Broad Institute), Justin Abreu(Broad Institute), Andrew J. Barry(Broad Institute), Tim Fennell(Broad Institute), Eric Banks(Broad Institute), Lauren Ambrogio(Broad Institute), Kristian Cibulskis(Broad Institute), Andrew Kernytsky(Broad Institute), Elena González(Broad Institute), Nicholas Rudzicz(McGill University), James C. Engert(McGill University), Mark A. DePristo(Broad Institute), Mark J. Daly(Broad Institute), Jonathan C. Cohen(The University of Texas Southwestern Medical Center), Helen H. Hobbs(The University of Texas Southwestern Medical Center), David Altshuler(Broad Institute), Gustav Schonfeld(Washington University in St. Louis), Stacey Gabriel(Broad Institute), Pin Yue(Washington University in St. Louis), Sekar Kathiresan(Broad Institute)

New England Journal of Medicine

October 13, 2010

10.1056/nejmoa1002926

Cited by 774Open Access

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Abstract

We sequenced all protein-coding regions of the genome (the "exome") in two family members with combined hypolipidemia, marked by extremely low plasma levels of low-density lipoprotein (LDL) cholesterol, high-density lipoprotein (HDL) cholesterol, and triglycerides. These two participants were compound heterozygotes for two distinct nonsense mutations in ANGPTL3 (encoding the angiopoietin-like 3 protein). ANGPTL3 has been reported to inhibit lipoprotein lipase and endothelial lipase, thereby increasing plasma triglyceride and HDL cholesterol levels in rodents. Our finding of ANGPTL3 mutations highlights a role for the gene in LDL cholesterol metabolism in humans and shows the usefulness of exome sequencing for identification of novel genetic causes of inherited disorders. (Funded by the National Human Genome Research Institute and others.).

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Exome Sequencing,<i>ANGPTL3</i>Mutations, and Familial Combined Hypolipidemia

Abstract

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