Stable Isotope Kinetic Study of ApoM (Apolipoprotein M).

Croyal, Mikaël; Billon-Crossouard, Stéphanie; Goulitquer, Sophie; Aguesse, Audrey; León, Luis; Fall, Fanta; Chétiveaux, Maud; Moyon, Thomas; Blanchard, Valentin; Ouguerram, Khadija; Lambert, Gilles; Nobécourt, Estelle; Krempf, Michel

Croyal, Mikaël; Billon-Crossouard, Stéphanie; Goulitquer, Sophie; Aguesse, Audrey; León, Luis; Fall, Fanta; Chétiveaux, Maud; Moyon, Thomas; Blanchard, Valentin; Ouguerram, Khadija; Lambert, Gilles; Nobécourt, Estelle; Krempf, Michel.

Afiliación

Croyal M; From the INRA, UMR 1280, CHU Hôtel-Dieu, Faculty of Medicine, University of Nantes, France (M.C., S.B.-C., A.A., L.L., F.F., T.M., K.O., E.N., M.K.); CRNHO, West Human Nutrition Research Center, Nantes, France (M.C., S.B.-C., A.A., F.F., M.C., V.B., K.O., E.N., M.K.); INSERM-UBO, UMR 1078-ECLA, IBSA
Billon-Crossouard S; From the INRA, UMR 1280, CHU Hôtel-Dieu, Faculty of Medicine, University of Nantes, France (M.C., S.B.-C., A.A., L.L., F.F., T.M., K.O., E.N., M.K.); CRNHO, West Human Nutrition Research Center, Nantes, France (M.C., S.B.-C., A.A., F.F., M.C., V.B., K.O., E.N., M.K.); INSERM-UBO, UMR 1078-ECLA, IBSA
Goulitquer S; From the INRA, UMR 1280, CHU Hôtel-Dieu, Faculty of Medicine, University of Nantes, France (M.C., S.B.-C., A.A., L.L., F.F., T.M., K.O., E.N., M.K.); CRNHO, West Human Nutrition Research Center, Nantes, France (M.C., S.B.-C., A.A., F.F., M.C., V.B., K.O., E.N., M.K.); INSERM-UBO, UMR 1078-ECLA, IBSA
Aguesse A; From the INRA, UMR 1280, CHU Hôtel-Dieu, Faculty of Medicine, University of Nantes, France (M.C., S.B.-C., A.A., L.L., F.F., T.M., K.O., E.N., M.K.); CRNHO, West Human Nutrition Research Center, Nantes, France (M.C., S.B.-C., A.A., F.F., M.C., V.B., K.O., E.N., M.K.); INSERM-UBO, UMR 1078-ECLA, IBSA
León L; From the INRA, UMR 1280, CHU Hôtel-Dieu, Faculty of Medicine, University of Nantes, France (M.C., S.B.-C., A.A., L.L., F.F., T.M., K.O., E.N., M.K.); CRNHO, West Human Nutrition Research Center, Nantes, France (M.C., S.B.-C., A.A., F.F., M.C., V.B., K.O., E.N., M.K.); INSERM-UBO, UMR 1078-ECLA, IBSA
Fall F; From the INRA, UMR 1280, CHU Hôtel-Dieu, Faculty of Medicine, University of Nantes, France (M.C., S.B.-C., A.A., L.L., F.F., T.M., K.O., E.N., M.K.); CRNHO, West Human Nutrition Research Center, Nantes, France (M.C., S.B.-C., A.A., F.F., M.C., V.B., K.O., E.N., M.K.); INSERM-UBO, UMR 1078-ECLA, IBSA
Chétiveaux M; From the INRA, UMR 1280, CHU Hôtel-Dieu, Faculty of Medicine, University of Nantes, France (M.C., S.B.-C., A.A., L.L., F.F., T.M., K.O., E.N., M.K.); CRNHO, West Human Nutrition Research Center, Nantes, France (M.C., S.B.-C., A.A., F.F., M.C., V.B., K.O., E.N., M.K.); INSERM-UBO, UMR 1078-ECLA, IBSA
Moyon T; From the INRA, UMR 1280, CHU Hôtel-Dieu, Faculty of Medicine, University of Nantes, France (M.C., S.B.-C., A.A., L.L., F.F., T.M., K.O., E.N., M.K.); CRNHO, West Human Nutrition Research Center, Nantes, France (M.C., S.B.-C., A.A., F.F., M.C., V.B., K.O., E.N., M.K.); INSERM-UBO, UMR 1078-ECLA, IBSA
Blanchard V; From the INRA, UMR 1280, CHU Hôtel-Dieu, Faculty of Medicine, University of Nantes, France (M.C., S.B.-C., A.A., L.L., F.F., T.M., K.O., E.N., M.K.); CRNHO, West Human Nutrition Research Center, Nantes, France (M.C., S.B.-C., A.A., F.F., M.C., V.B., K.O., E.N., M.K.); INSERM-UBO, UMR 1078-ECLA, IBSA
Ouguerram K; From the INRA, UMR 1280, CHU Hôtel-Dieu, Faculty of Medicine, University of Nantes, France (M.C., S.B.-C., A.A., L.L., F.F., T.M., K.O., E.N., M.K.); CRNHO, West Human Nutrition Research Center, Nantes, France (M.C., S.B.-C., A.A., F.F., M.C., V.B., K.O., E.N., M.K.); INSERM-UBO, UMR 1078-ECLA, IBSA
Lambert G; From the INRA, UMR 1280, CHU Hôtel-Dieu, Faculty of Medicine, University of Nantes, France (M.C., S.B.-C., A.A., L.L., F.F., T.M., K.O., E.N., M.K.); CRNHO, West Human Nutrition Research Center, Nantes, France (M.C., S.B.-C., A.A., F.F., M.C., V.B., K.O., E.N., M.K.); INSERM-UBO, UMR 1078-ECLA, IBSA
Nobécourt E; From the INRA, UMR 1280, CHU Hôtel-Dieu, Faculty of Medicine, University of Nantes, France (M.C., S.B.-C., A.A., L.L., F.F., T.M., K.O., E.N., M.K.); CRNHO, West Human Nutrition Research Center, Nantes, France (M.C., S.B.-C., A.A., F.F., M.C., V.B., K.O., E.N., M.K.); INSERM-UBO, UMR 1078-ECLA, IBSA
Krempf M; From the INRA, UMR 1280, CHU Hôtel-Dieu, Faculty of Medicine, University of Nantes, France (M.C., S.B.-C., A.A., L.L., F.F., T.M., K.O., E.N., M.K.); CRNHO, West Human Nutrition Research Center, Nantes, France (M.C., S.B.-C., A.A., F.F., M.C., V.B., K.O., E.N., M.K.); INSERM-UBO, UMR 1078-ECLA, IBSA

Arterioscler Thromb Vasc Biol ; 38(1): 255-261, 2018 01.

Article en En | MEDLINE | ID: mdl-29146748

ABSTRACT

ABSTRACT

OBJECTIVE:

ApoM (apolipoprotein M) binds primarily to high-density lipoprotein before to be exchanged with apoB (apolipoprotein B)-containing lipoproteins. Low-density lipoprotein (LDL) receptor-mediated clearance of apoB-containing particles could influence plasma apoM kinetics and decrease its antiatherogenic properties. In humans, we aimed to describe the interaction of apoM kinetics with other components of lipid metabolism to better define its potential benefit on atherosclerosis. APPROACH AND

RESULTS:

Fourteen male subjects received a primed infusion of 2H3-leucine for 14 hours, and analyses were performed by liquid chromatography-tandem mass spectrometry from the hourly plasma samples. Fractional catabolic rates and production rates within lipoproteins were calculated using compartmental models. ApoM was found not only in high-density lipoprotein (59%) and LDL (4%) but also in a non-lipoprotein-related compartment (37%). The apoM distribution was heterogeneous within LDL and non-lipoprotein-related compartments according to plasma triglycerides (r=0.86; P<0.001). The relationships between sphingosine-1-phosphate and apoM were confirmed in all compartments (r range, 0.55-0.89; P<0.05). ApoM fractional catabolic rates and production rates were 0.16±0.07 pool/d and 0.14±0.06 mg/kg per day in high-density lipoprotein and 0.56±0.10 pool/d and 0.03±0.01 mg/kg per day in LDL, respectively. Fractional catabolic rates of LDL-apoM and LDL-apoB100 were correlated (r=0.55; P=0.042). Significant correlations were found between triglycerides and production rates of LDL-apoM (r=0.73; P<0.004).

CONCLUSIONS:

In humans, LDL kinetics play a key role in apoM turnover. Plasma triglycerides act on both apoM and sphingosine-1-phosphate distributions between lipoproteins. These results confirmed that apoM could be bound to high-density lipoprotein after secretion and then quickly exchanged with a non-lipoprotein-related compartment and to LDL to be slowly catabolized.

Asunto(s)

Apolipoproteínas M/sangre; Deuterio/administración & dosificación; Leucina/administración & dosificación; Adolescente; Adulto; Cromatografía Líquida de Alta Presión; Cromatografía Liquida; Humanos; Infusiones Intravenosas; Cinética; Lipoproteínas HDL/sangre; Lipoproteínas LDL/sangre; Lisofosfolípidos/sangre; Masculino; Persona de Mediana Edad; Unión Proteica; Proteolisis; Esfingosina/análogos & derivados; Esfingosina/sangre; Triglicéridos/sangre; Adulto Joven

Palabras clave

apolipoproteins; lipid metabolism; lipoproteins; sphingosine-1-phosphate; triglycerides

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Texto completo: 1 Colección: 01-internacional Base de datos: MEDLINE Asunto principal: Deuterio / Apolipoproteínas M / Leucina Límite: Adolescent / Adult / Humans / Male / Middle aged Idioma: En Revista: Arterioscler Thromb Vasc Biol Asunto de la revista: ANGIOLOGIA Año: 2018 Tipo del documento: Article

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