Identification of a Gain-of-Function <i>LIPC</i> Variant as a Novel Cause of Familial Combined Hypocholesterolemia.

Dijk, Wieneke; Di Filippo, Mathilde; Kooijman, Sander; van Eenige, Robin; Rimbert, Antoine; Caillaud, Amandine; Thedrez, Aurélie; Arnaud, Lucie; Pronk, Amanda; Garçon, Damien; Sotin, Thibaud; Lindenbaum, Pierre; Ozcariz Garcia, Enrique; Pais de Barros, Jean-Paul; Duvillard, Laurence; Si-Tayeb, Karim; Amigo, Nuria; Le Questel, Jean-Yves; Rensen, Patrick C N; Le May, Cédric; Moulin, Philippe; Cariou, Bertrand

Identification of a Gain-of-Function LIPC Variant as a Novel Cause of Familial Combined Hypocholesterolemia.

Dijk, Wieneke; Di Filippo, Mathilde; Kooijman, Sander; van Eenige, Robin; Rimbert, Antoine; Caillaud, Amandine; Thedrez, Aurélie; Arnaud, Lucie; Pronk, Amanda; Garçon, Damien; Sotin, Thibaud; Lindenbaum, Pierre; Ozcariz Garcia, Enrique; Pais de Barros, Jean-Paul; Duvillard, Laurence; Si-Tayeb, Karim; Amigo, Nuria; Le Questel, Jean-Yves; Rensen, Patrick C N; Le May, Cédric; Moulin, Philippe; Cariou, Bertrand.

Dijk W; Nantes Université, CHU Nantes, CNRS, INSERM, l'institut du thorax, France (W.D., A.R., A.C., A.T., L.A., D.G., T.S., P.L., K.S.-T., C.L.M., B.C.).
Di Filippo M; UF Dyslipidémies, Service de Biochimie et de Biologie Moléculaire, Laboratoire de Biologie Médicale MultiStites, Hospices Civils de Lyon, Bron, France (M.D.F.).
Kooijman S; CarMen Laboratory, INSERM, INRA, INSA Lyon, Université Claude Bernard Lyon 1, Pierre-Bénite, France (M.D.F., P.M.).
van Eenige R; Department of Medicine, Division of Endocrinology and Einthoven Laboratory for Experimental Vascular Medicine, Leiden University Medical Center, the Netherlands (S.K., R.v.E., A.P., P.C.N.R.).
Rimbert A; Department of Medicine, Division of Endocrinology and Einthoven Laboratory for Experimental Vascular Medicine, Leiden University Medical Center, the Netherlands (S.K., R.v.E., A.P., P.C.N.R.).
Caillaud A; Nantes Université, CHU Nantes, CNRS, INSERM, l'institut du thorax, France (W.D., A.R., A.C., A.T., L.A., D.G., T.S., P.L., K.S.-T., C.L.M., B.C.).
Thedrez A; Nantes Université, CHU Nantes, CNRS, INSERM, l'institut du thorax, France (W.D., A.R., A.C., A.T., L.A., D.G., T.S., P.L., K.S.-T., C.L.M., B.C.).
Arnaud L; Nantes Université, CHU Nantes, CNRS, INSERM, l'institut du thorax, France (W.D., A.R., A.C., A.T., L.A., D.G., T.S., P.L., K.S.-T., C.L.M., B.C.).
Pronk A; Nantes Université, CHU Nantes, CNRS, INSERM, l'institut du thorax, France (W.D., A.R., A.C., A.T., L.A., D.G., T.S., P.L., K.S.-T., C.L.M., B.C.).
Garçon D; Department of Medicine, Division of Endocrinology and Einthoven Laboratory for Experimental Vascular Medicine, Leiden University Medical Center, the Netherlands (S.K., R.v.E., A.P., P.C.N.R.).
Sotin T; Nantes Université, CHU Nantes, CNRS, INSERM, l'institut du thorax, France (W.D., A.R., A.C., A.T., L.A., D.G., T.S., P.L., K.S.-T., C.L.M., B.C.).
Lindenbaum P; Nantes Université, CHU Nantes, CNRS, INSERM, l'institut du thorax, France (W.D., A.R., A.C., A.T., L.A., D.G., T.S., P.L., K.S.-T., C.L.M., B.C.).
Ozcariz Garcia E; Nantes Université, CHU Nantes, CNRS, INSERM, l'institut du thorax, France (W.D., A.R., A.C., A.T., L.A., D.G., T.S., P.L., K.S.-T., C.L.M., B.C.).
Pais de Barros JP; Biosfer Teslab, Reus, Spain (E.O.G., N.A.).
Duvillard L; Lipidomic Platform, INSERM UMR1231, Université de Bourgogne Franche-Comté, Dijon, France (J.-P.P.d.B.).
Si-Tayeb K; University of Burgundy, INSERM LNC UMR1231, Dijon, France (L.D.).
Amigo N; CHU Dijon, Department of Biochemistry, Dijon, France (L.D.).
Le Questel JY; Nantes Université, CHU Nantes, CNRS, INSERM, l'institut du thorax, France (W.D., A.R., A.C., A.T., L.A., D.G., T.S., P.L., K.S.-T., C.L.M., B.C.).
Rensen PCN; Biosfer Teslab, Reus, Spain (E.O.G., N.A.).
Le May C; Department of Basic Medical Sciences, Rovira I Virgili University, IISPV, CIBERDEM, Reus, Spain (N.A.).
Moulin P; Nantes Université, CNRS, CEISAM, UMR 6230, Nantes, France (J.-Y.L.Q.).
Cariou B; Department of Medicine, Division of Endocrinology and Einthoven Laboratory for Experimental Vascular Medicine, Leiden University Medical Center, the Netherlands (S.K., R.v.E., A.P., P.C.N.R.).

Circulation ; 146(10): 724-739, 2022 09 06.

Article en En | MEDLINE | ID: mdl-35899625

ABSTRACT

ABSTRACT

BACKGROUND:

Atherosclerotic cardiovascular disease is the main cause of mortality worldwide and is strongly influenced by circulating low-density lipoprotein (LDL) cholesterol levels. Only a few genes causally related to plasma LDL cholesterol levels have been identified so far, and only 1 gene, ANGPTL3, has been causally related to combined hypocholesterolemia. Here, our aim was to elucidate the genetic origin of an unexplained combined hypocholesterolemia inherited in 4 generations of a French family.

METHODS:

Using next-generation sequencing, we identified a novel dominant rare variant in the LIPC gene, encoding for hepatic lipase, which cosegregates with the phenotype. We characterized the impact of this LIPC-E97G variant on circulating lipid and lipoprotein levels in family members using nuclear magnetic resonance-based lipoprotein profiling and lipidomics. To uncover the mechanisms underlying the combined hypocholesterolemia, we used protein homology modeling, measured triglyceride lipase and phospholipase activities in cell culture, and studied the phenotype of APOE*3.Leiden.CETP mice after LIPC-E97G overexpression.

RESULTS:

Family members carrying the LIPC-E97G variant had very low circulating levels of LDL cholesterol and high-density lipoprotein cholesterol, LDL particle numbers, and phospholipids. The lysophospholipids/phospholipids ratio was increased in plasma of LIPC-E97G carriers, suggestive of an increased lipolytic activity on phospholipids. In vitro and in vivo studies confirmed that the LIPC-E97G variant specifically increases the phospholipase activity of hepatic lipase through modification of an evolutionarily conserved motif that determines substrate access to the hepatic lipase catalytic site. Mice overexpressing human LIPC-E97G recapitulated the combined hypocholesterolemic phenotype of the family and demonstrated that the increased phospholipase activity promotes catabolism of triglyceride-rich lipoproteins by different extrahepatic tissues but not the liver.

CONCLUSIONS:

We identified and characterized a novel rare variant in the LIPC gene in a family who presents with dominant familial combined hypocholesterolemia. This gain-of-function variant makes LIPC the second identified gene, after ANGPTL3, causally involved in familial combined hypocholesterolemia. Our mechanistic data highlight the critical role of hepatic lipase phospholipase activity in LDL cholesterol homeostasis and suggest a new LDL clearance mechanism.

Asunto(s)

Mutación con Ganancia de Función; Lipasa; Proteína 3 Similar a la Angiopoyetina; Proteínas Similares a la Angiopoyetina/genética; Animales; HDL-Colesterol; LDL-Colesterol; Humanos; Lipasa/genética; Lipoproteínas; Ratones; Fosfolipasas/genética

Palabras clave

LIPC protein, human; Lipc protein, mouse; cholesterol, HDL; cholesterol, LDL; phospholipases

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Texto completo: 1 Banco de datos: MEDLINE Asunto principal: Mutación con Ganancia de Función / Lipasa Tipo de estudio: Diagnostic_studies Límite: Animals / Humans Idioma: En Año: 2022 Tipo del documento: Article

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