文化大學機構典藏 CCUR:Item 987654321/44619
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    Please use this identifier to cite or link to this item: https://irlib.pccu.edu.tw/handle/987654321/44619


    Title: Pleiotropic association of LIPC variants with lipid and urinary 8-hydroxy deoxyguanosine levels in a Taiwanese population
    Authors: Teng, MS (Teng, Ming-Sheng)
    Wu, S (Wu, Semon)
    Hsu, LA (Hsu, Lung-An)
    Tzeng, IS (Tzeng, I-Shiang)
    Chou, HH (Chou, Hsin-Hua)
    Su, CW (Su, Cheng-Wen)
    Ko, YL (Ko, Yu-Lin)
    Contributors: 生命科學系
    Keywords: HEPATIC LIPASE GENE
    GENOME-WIDE ASSOCIATION
    CORONARY-HEART-DISEASE
    OXIDATIVE DNA-DAMAGE
    DENSITY-LIPOPROTEIN
    CARDIOVASCULAR-DISEASE
    METABOLIC SYNDROME
    CHOLESTEROL LEVELS
    RISK;SUSCEPTIBILITY
    Date: 2019-05-10
    Issue Date: 2019-06-18 11:56:11 (UTC+8)
    Abstract: BackgroundHepatic lipase (HL, encoded by LIPC) is a glycoprotein primarily synthesized and secreted by hepatocytes. Previous studies had demonstrated that HL is crucial for reverse cholesterol transport and affects the metabolism, composition, and level of several lipoproteins. In current study, we investigated the association of LIPC (Lipase C, Hepatic Type) variants with circulating and urinary biomarker levels by using subgroup and mediation analyses.MethodsA total of 572 participants from Taiwan were genotyped for three LIPC single nucleotide polymorphisms (SNPs) by using TaqMan assay. Fasting levels of glucose, lipid profile, inflammation markers, urine creatinine and 8-hydroxy deoxyguanosine (8-OHdG) were measured. The chi-square test, 2-sample t test and Analysis of variance (ANOVA) were used to examine differences among variables and genotype frequencies.ResultsSNPs rs2043085 and rs1532085 were significantly associated with urinary 8-OHdG levels, whereas all three SNPs were more significantly associated with Triglycerides (TG) or HDL-cholesterol (HDL-C) levels after additional adjustment for HDL-C or TG levels, respectively. Subgroup analyses revealed that the association of the LIPC SNPs with the levels of serum TG, HDL-C, and urinary 8-OHdG were predominantly observed in the men but not in the women. Differential associations of the LIPC SNPs with various lipid levels were observed in participants with different adiposity statuses. Mediation analyses indicated that TG levels acted as a suppressor masking the association of the LIPC genotypes with HDL-C levels, particularly in the men (Sobel test, all P<0.01).ConclusionOur data revealed that interaction and suppression effects mediated the pleiotropic association of the LIPC variants. The effects of the LIPC SNPs depended on sex, adiposity status, and TG levels. Thus, our findings can provide a method for identifying high-risk populations of cardiovascular diseases for clinical diagnosis.
    Appears in Collections:[Department of Biology ] journal articles

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