Trimethylamine N-oxide and the reverse cholesterol transport in cardiovascular disease: a cross-sectional study

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作者
Laura Bordoni
Joanna J. Samulak
Angelika K. Sawicka
Iwona Pelikant-Malecka
Adrianna Radulska
Lukasz Lewicki
Leszek Kalinowski
Rosita Gabbianelli
Robert A. Olek
机构
[1] University of Camerino,Unit of Molecular Biology, School of Pharmacy
[2] Via Gentile III da Varano,Doctoral School
[3] Gdansk University of Physical Education and Sport,Department of Human Physiology, Faculty of Health Sciences
[4] Medical University of Gdansk,Department of Medical Laboratory Diagnostics
[5] Medical University of Gdansk,Department of Mechanics of Materials and Structures
[6] Biobanking and Biomolecular Resources Research Infrastructure Poland (BBMRI.PL),undefined
[7] University Center for Cardiology,undefined
[8] Gdansk University of Technology,undefined
[9] Poznan University of Physical Education,undefined
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Scientific Reports | / 10卷
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摘要
The early atherosclerotic lesions develop by the accumulation of arterial foam cells derived mainly from cholesterol-loaded macrophages. Therefore, cholesterol and cholesteryl ester transfer protein (CETP) have been considered as causative in atherosclerosis. Moreover, recent studies indicate the role of trimethylamine N-oxide (TMAO) in development of cardiovascular disease (CVD). The current study aimed to investigate the association between TMAO and CETP polymorphisms (rs12720922 and rs247616), previously identified as a genetic determinant of circulating CETP, in a population of coronary artery disease (CAD) patients (n = 394) and control subjects (n = 153). We also considered age, sex, trimethylamine (TMA) levels and glomerular filtration rate (GFR) as other factors that can potentially play a role in this complex picture. We found no association of TMAO with genetically determined CETP in a population of CAD patients and control subjects. Moreover, we noticed no differences between CAD patients and control subjects in plasma TMAO levels. On the contrary, lower levels of TMA in CAD patients respect to controls were observed. Our results indicated a significant correlation between GFR and TMAO, but not TMA. The debate whether TMAO can be a harmful, diagnostic or protective marker in CVD needs to be continued.
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