Publication | Open Access
Catabolic rate of low density lipoprotein is influenced by variation in the apolipoprotein B gene.
68
Citations
32
References
1988
Year
Metabolic SyndromeApolipoprotein B GeneBiochemistryGeneticsPhysiologyGenetic EpidemiologyLdl Kinetic ParametersHuman PolymorphismLdl Receptor GeneHyperlipidemiaLipoprotein MetabolismCatabolic RateLdl ReceptorDyslipidemiaLow Density LipoproteinHealth Sciences
This study examines the potential influence of genetic variation on the metabolism of LDL. Restriction fragment length polymorphisms (RFLP) of the gene coding for apo B were identified using the endonucleases Xba I, Eco RI, and Msp I in a group of 19 subjects with moderate hyperlipidemia. There was a significant association between the Xba I polymorphism and the total fractional clearance rate (FCR) of LDL. The individuals with the X1X1 genotype had, on average, a 22% higher FCR (P less than 0.025) than those with the genotype X2X2 (X2 allele = presence of Xba I cutting site). This difference was attributable to increased clearance by the receptor-mediated pathway of LDL catabolism. In this group of subjects, there was no association of LDL kinetic parameters and RFLPs of the LDL receptor gene or the AI- CIII- AIV gene cluster. The data suggest that variation in apo B itself, presumably acting through variable binding to the LDL receptor, makes a significant contribution to the rate of catabolism of LDL.
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