自身免疫
医学
免疫学
免疫系统
系统性红斑狼疮
载脂蛋白B
疾病
胆固醇
内科学
作者
Ingrid Yao Mattisson,Sara Rattik,Harry Björkbacka,Irena Ljungcrantz,Manuela Terrinoni,Michael Lebens,Jan Holmgren,Gunilla Nordin Fredrikson,Birgitta Gullstrand,Anders Bengtsson,Jan Nilsson,Maria Wigren
标识
DOI:10.1016/j.vph.2021.106863
摘要
Patients suffering from systemic lupus erythematosus (SLE) are at increased risk of developing cardiovascular disease (CVD) and traditional therapies including statins provide insufficient protection. Impaired removal of apoptotic material is a common pathogenic mechanism in both SLE and atherosclerosis and is considered to be a key factor in the development of autoimmunity. Since oxidized LDL and apoptotic material bind to the same receptors, we aimed to investigate if targeting the oxidized LDL autoimmunity can affect atherosclerosis in SLE. To investigate the possible role of oxidized LDL autoimmunity in the accelerated atherosclerosis associated with SLE we used a hypercholesterolemic SLE mouse model (B6.lpr.ApoE-/- mice). Promoting LDL tolerance through mucosal immunization with an apolipoprotein B-100 peptide p45 (amino acids 661-680) and cholera toxin B-subunit fusion protein increased regulatory T cells and B cells in mesenteric lymph nodes and reduced plaque development in the aorta by 33%. Treatment with the oxidized LDL-specific antibody Orticumab reduced aortic atherosclerosis by 43%, subvalvular plaque area by 50% and the macrophage content by 31%. The present study provides support for oxLDL as a possible target for prevention of cardiovascular complications in SLE.
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