4.7 Article

Malondialdehyde-modified HDL particles elicit a specific IgG response in abdominal aortic aneurysm

Journal

FREE RADICAL BIOLOGY AND MEDICINE
Volume 174, Issue -, Pages 171-181

Publisher

ELSEVIER SCIENCE INC
DOI: 10.1016/j.freeradbiomed.2021.08.004

Keywords

HDL; MDA; Oxidative stress; Immune response; Antibodies; Abdominal aortic aneurysm

Funding

  1. Spanish MINECO [SAF2016-80843-R, PID2019-106814RB-I00, PGC2018-097019-B-I00]
  2. CAM (Com-plemento II-CM) [S2017/BMD-3673]
  3. Fondo de Investigaciones Sani-tarias ISCIII-FEDER [PI19/00128, Biobancos RD09/0076/00101, PI16/00113, PT17/0019/0003-ISCIII-SGEFI/ERDF]
  4. FEDER Una manera de hacer Europa
  5. la Caixa Banking Foundation [HR17-00247]

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The study found that oxidative modifications could lead to dysfunctional HDL in abdominal aortic aneurysm (AAA), and antibodies against HDL-MDA have the potential to be used as stable biomarkers of oxidative stress in AAA patients. These antibodies were detected in both a mouse model and AAA patients.
High Density Lipoprotein (HDL) plays a protective role in abdominal aortic aneurysm (AAA); however, recent findings suggest that oxidative modifications could lead to dysfunctional HDL in AAA. This study aimed at testing the effect of oxidized HDL on aortic lesions and humoral immune responses in a mouse model of AAA induced by elastase, and evaluating whether antibodies against modified HDL can be found in AAA patients. HDL particles were oxidized with malondialdehyde (HDL-MDA) and the changes were studied by biochemical and proteomics approaches. Experimental AAA was induced in mice by elastase perfusion and then mice were treated with HDL-MDA, HDL or vehicle for 14 days. Aortic lesions were studied by histomorphometric analysis. Levels of anti-HDL-MDA IgG antibodies were measured by an in-house immunoassay in the mouse model, in human tissue-supernatants and in plasma samples from the VIVA cohort. HDL oxidation with MDA was confirmed by enhanced susceptibility to diene formation. Proteomics demonstrated the presence of MDA adducts on Lysine residues of HDL proteins, mainly ApoA-I. MDA-modification of HDL abrogated the protective effect of HDL on cultured endothelial cells as well as on AAA dilation in mice. Exposure to HDL-MDA elicited an anti-HDL-MDA IgG response in mice. Anti-HDL-MDA were also detected in tissue-conditioned media from AAA patients, mainly in intraluminal thrombus. Higher plasma levels of anti-HDLMDA IgG antibodies were found in AAA patients compared to controls. Anti-HDL-MDA levels were associated with smoking and were independent predictors of overall mortality in AAA patients. Overall, MDA-oxidized HDL trigger a specific humoral immune response in mice. Besides, antibodies against HDL-MDA can be detected in tissue and plasma of AAA patients, suggesting its potential use as surrogate stable biomarkers of oxidative stress in AAA.

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