Serum Apolipoprotein J in Health, Coronary Heart Disease and Type 2 Diabetes Mellitus

Overview

Journal J Atheroscler Thromb

Date 2006 Dec 29

PMID 17192696

Citations 21

Authors

Takeshi Kujiraoka

Hiroaki Hattori

Yoshikazu Miwa

Mitsuaki Ishihara

Takahiro Ueno

Jun Ishii

Masahiro Tsuji

Tadao Iwasaki

Yoshiyuki Sasaguri

Takayuki Fujioka

Satoshi Saito

Motoo Tsushima

Taro Maruyama

Irina P Miller

Norman E Miller

Tohru Egashira

Affiliations

Soon will be listed here.

Abstract

Apolipoprotein (apo) J, clusterin, is ubiquitously expressed in many tissues, and is a component of high-density lipoproteins (HDLs). There is experimental evidence that it may be anti-atherogenic through its effects on cholesterol transport, smooth muscle cell proliferation and lipid peroxidation. HDLs containing apo J and apo A-I carry paraoxonase (PON1), which protects low-density lipoproteins from oxidative modification; however, the extent to which apo J affects coronary heart disease (CHD) is not known. We have developed a sandwich ELISA that enables apo J to be assayed in the range of 13-200 microg/mL. Serum apo J was 52.8+/-0.8 microg/mL (mean+/-SEM; range, 36.0-84.3 microg/mL; n=92) in healthy Japanese men, and 49.3+/-0.5 microg/mL (34.5-72.8; n=241) in healthy Japanese women. Multiple regression of these data and results from 67 men with CHD showed that apo J concentration was unrelated to age, sex or body mass index, but was positively related to serum PON1 (p<0.001) and apo B (p<0.02) concentrations. In women, it was also positively related to blood glucose (p<0.02). After adjusting for its associations with covariates, serum apo J averaged 5.4 microg/mL, lower in CHD men than in controls (p<0.003). Type 2 diabetics had higher apo J concentrations (men, 83.1+/-3.4 microg/mL, n=64; women, 64.0+/-2.3 microg/mL, n=46) than healthy men and women (p<0.001). In these Type 2 diabetics, apo J concentration was unrelated to PON1 concentration, but was positively related to blood glucose (p<0.01). After adjustment for its relation to blood glucose, the mean apo J concentration was similar in diabetics and healthy subjects. These findings suggest that apo J may be anti-atherogenic in humans, and that its concentration is raised by Type 2 diabetes.

Citing Articles

Clusterin Plasma Concentrations Are Decreased in Sepsis and Inversely Correlated with Established Markers of Inflammation.

Yagmur E, Abu Jhaisha S, Buendgens L, Sapundzhieva N, Brozat J, Hohlstein P Diagnostics (Basel). 2022; 12(12).

PMID: 36553017 PMC: 9776480. DOI: 10.3390/diagnostics12123010.

The Influence of Clusterin Glycosylation Variability on Selected Pathophysiological Processes in the Human Body.

Janiszewska E, Kmieciak A, Kacperczyk M, Witkowska A, Kratz E Oxid Med Cell Longev. 2022; 2022:7657876.

PMID: 36071866 PMC: 9441386. DOI: 10.1155/2022/7657876.

Association of clusterin with the BRI2-derived amyloid molecules ABri and ADan.

Rostagno A, Calero M, Holton J, Revesz T, Lashley T, Ghiso J Neurobiol Dis. 2021; 158:105452.

PMID: 34298087 PMC: 8440498. DOI: 10.1016/j.nbd.2021.105452.

Sterol O-acyltransferase 2 chaperoned by apolipoprotein J facilitates hepatic lipid accumulation following viral and nutrient stresses.

Sun H, Chen T, Tan Y, Wang C, Young K Commun Biol. 2021; 4(1):564.

PMID: 33980978 PMC: 8115332. DOI: 10.1038/s42003-021-02093-2.

Circulating IL-6, clusterin and irisin in obese subjects with different grades of obesity: association with insulin resistance and sexual dimorphism.

Werida R, El-Gharbawy N, Mostafa T Arch Endocrinol Metab. 2021; 65(2):126-136.

PMID: 33905632 PMC: 10065324. DOI: 10.20945/2359-3997000000336.