Rare genetic variants with large effect on triglycerides in subjects with a clinical diagnosis of familial vs nonfamilial hypertriglyceridemia

Rare genetic variants with large effect on triglycerides in subjects with a clinical diagnosis of familial vs nonfamilial hypertriglyceridemia

Most primary severe hypertriglyceridemias (HTGs) are diagnosed in adults, but their molecular foundations have not been completely elucidated. We aimed to identify rare dysfunctional mutations in genes encoding regulators of lipoprotein lipase (LPL) function in patients with familial and non-familia...

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Veröffentlicht in:Journal of clinical lipidology 2016-07, Vol.10 (4), p.790-797
Hauptverfasser: De Castro-Orós, Isabel, Civeira, Fernando, Pueyo, María Jesús, Mateo-Gallego, Rocío, Bolado-Carrancio, Alfonso, Lamíquiz-Moneo, Itziar, Álvarez-Sala, Luis, Fabiani, Fernando, Cofán, Montserrat, Cenarro, Ana, Rodríguez-Rey, José Carlos, Ros, Emilio, Pocoví, Miguel
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Sprache:eng
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Adolescent
Adult
Aged
APOA5
Base Sequence
Female
Genetic Variation
GPIHBP1
Humans
Hyperlipoproteinemia Type IV - blood
Hyperlipoproteinemia Type IV - diagnosis
Hyperlipoproteinemia Type IV - genetics
Hypertriglyceridemia
LMF1
LPL
Male
Middle Aged
Mutation
Triglycerides - blood
Young Adult
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Zusammenfassung:Most primary severe hypertriglyceridemias (HTGs) are diagnosed in adults, but their molecular foundations have not been completely elucidated. We aimed to identify rare dysfunctional mutations in genes encoding regulators of lipoprotein lipase (LPL) function in patients with familial and non-familial primary HTG. We sequenced promoters, exons, and exon–intron boundaries of LPL, APOA5, LMF1, and GPIHBP1 in 118 patients with severe primary HTG (triglycerides >500 mg/dL) and 53 normolipidemic controls. Variant functionality was analyzed using predictive software and functional assays for mutations in regulatory regions. We identified 29 rare variants, 10 of which had not been previously described: c.(-16A>G), c.(1018+2G>A), and p.(His80Arg) in LPL; p.(Arg143Alafs*57) in APOA5; p.(Val140Ile), p.(Leu235Ile), p.(Lys520*), and p.(Leu552Arg) in LMF1; and c.(-83G>A) and c.(-192A>G) in GPIHBP1. The c.(1018+2G>A) variant led to deletion of exon 6 in LPL cDNA, whereas the c.(-16A>G) analysis showed differences in the affinity for nuclear proteins. Overall, 20 (17.0%) of the patients carried at least one allele with a rare pathogenic variant in LPL, APOA5, LMF1, or GPIHBP1. The presence of a rare pathogenic variant was not associated with lipid values, family history of HTG, clinical diagnosis, or previous pancreatitis. Less than one in five subjects with triglycerides >500 mg/dL and no major secondary cause for HTG may carry a rare pathogenic mutation in LPL, APOA5, LMF1, or GPIHBP1. The presence of a rare pathogenic variant is not associated with a differential phenotype. •Subjects with familial and nonfamilial primary HTG were assessed for rare mutations.•In 118 subjects, 29 rare variants were identified; 7/10 novel ones were pathogenic.•We studied LPL, APOA5, LMF1, and GPIHBP1 variants in silico and in vitro.•Less than 20% carry a rare pathogenic mutation in LPL, APOA5, LMF1, or GPIHBP1.•No clinical information associates with a higher frequency of pathogenic mutations.
ISSN:1933-2874
1876-4789
DOI:10.1016/j.jacl.2016.02.010