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Citations to this article

Increased coronary heart disease in Japanese-American men with mutation in the cholesteryl ester transfer protein gene despite increased HDL levels.
S Zhong, … , J D Curb, A R Tall
S Zhong, … , J D Curb, A R Tall
Published June 15, 1996
Citation Information: J Clin Invest. 1996;97(12):2917-2923. https://doi.org/10.1172/JCI118751.
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Research Article Article has an altmetric score of 11

Increased coronary heart disease in Japanese-American men with mutation in the cholesteryl ester transfer protein gene despite increased HDL levels.

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Abstract

Plasma high density lipoprotein (HDL) levels are strongly genetically determined and show a general inverse relationship with coronary heart disease (CHD). The cholesteryl ester transfer protein (CETP) mediates the transfer of cholesteryl esters from HDL to other lipoproteins and is a key participant in the reverse transport of cholesterol from the periphery to the liver. A high prevalence of two different CETP gene mutations (D442G, 5.1%; intron 14G:A, 0.5%), was found in 3,469 men of Japanese ancestry in the Honolulu Heart Program and mutations were associated with decreased CETP (-35%) and increased HDL chol levels (+10% for D442G). However, the overall prevalence of definite CHD was 21% in men with mutations and 16% in men without mutations. The relative risk (RR) of CHD was 1.43 in men with mutations (P < .05); after adjustment for CHD risk factors, the RR was 1.55 (P = .02); after additional adjustment for HDL levels, the RR was 1.68 (P = .008). Similar RR values were obtained for the D442G mutation alone. Increased CHD in men with mutations was primarily observed for HDL chol 41-60 mg/dl; for HDL chol > 60 mg/dl men with and without mutations had low CHD prevalence. Thus, genetic CETP deficiency appears to be an independent risk factor for CHD, primarily due to increased CHD prevalence in men with the D442G mutation and HDL cholesterol between 41 and 60 mg/dl. The findings suggest that both HDL concentration and the dynamics of cholesterol transport through HDL (i.e., reverse cholesterol transport) determine the anti-atherogenicity of the HDL fraction.

Authors

S Zhong, D S Sharp, J S Grove, C Bruce, K Yano, J D Curb, A R Tall

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Citations to this article in year 2020 (11)

Title and authors Publication Year
Lipid Transfer in Lipoprotein Metabolism and Cardiovascular Disease
XC Jiang
2020
Lipid Transfer in Lipoprotein Metabolism and Cardiovascular Disease
XC Jiang
2020
Lipid Transfer in Lipoprotein Metabolism and Cardiovascular Disease
XC Jiang
2020
Lipid Transfer in Lipoprotein Metabolism and Cardiovascular Disease
XC Jiang
2020
Lipid Transfer in Lipoprotein Metabolism and Cardiovascular Disease
XC Jiang
2020
Lipid Transfer in Lipoprotein Metabolism and Cardiovascular Disease
XC Jiang
2020
Lipid Transfer in Lipoprotein Metabolism and Cardiovascular Disease
XC Jiang
2020
A Population-Based Cohort Study on the Association of Hyperthyroidism With the Risk of Hyperlipidemia and the Effects of Anti-thyroid Drugs on Hepatic Gene Expression
TY Wu, CH Wang, N Tien, CL Lin, FY Chu, HY Chang, YP Lim
Frontiers in Medicine 2020
The Alcohol–High-Density Lipoprotein Athero-Protective Axis
C Rosales, BK Gillard, AM Gotto, HJ Pownall
Biomolecules 2020
High‐density lipoprotein‐related cholesterol metabolism in Alzheimer’s disease
S Pedrini, P Chatterjee, E Hone, RN Martins
Journal of Neurochemistry 2020
Efficacy of oral rosuvastatin intervention on HDL and its associated proteins in men with type 2 diabetes mellitus
S Naresh, AR Bitla, PV Rao, A Sachan, YL Amancharla
Endocrine 2020

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