Department of Medicine, Cardiovascular Medicine, Vanderbilt University Medical Center, Nashville, TN, United States.
Department of Pharmacology, Vanderbilt University, Nashville, TN, United States.
Mol Metab. 2023 Jan;67:101651. doi: 10.1016/j.molmet.2022.101651. Epub 2022 Dec 5.
Oxidative stress contributes to the development of insulin resistance (IR) and atherosclerosis. Peroxidation of lipids produces reactive dicarbonyls such as Isolevuglandins (IsoLG) and malondialdehyde (MDA) that covalently bind plasma/cellular proteins, phospholipids, and DNA leading to altered function and toxicity. We examined whether scavenging reactive dicarbonyls with 5'-O-pentyl-pyridoxamine (PPM) protects against the development of IR and atherosclerosis in Ldlr mice.
Male or female Ldlr mice were fed a western diet (WD) for 16 weeks and treated with PPM versus vehicle alone. Plaque extent, dicarbonyl-lysyl adducts, efferocytosis, apoptosis, macrophage inflammation, and necrotic area were measured. Plasma MDA-LDL adducts and the in vivo and in vitro effects of PPM on the ability of HDL to reduce macrophage cholesterol were measured. Blood Ly6C monocytes and ex vivo 5-ethynyl-2'-deoxyuridine (EdU) incorporation into bone marrow CD11b+ monocytes and CD34+ hematopoietic stem and progenitor cells (HSPC) were also examined. IR was examined by measuring fasting glucose/insulin levels and tolerance to insulin/glucose challenge.
PPM reduced the proximal aortic atherosclerosis by 48% and by 46% in female and male Ldlr mice, respectively. PPM also decreased IR and hepatic fat and inflammation in male Ldlr mice. Importantly, PPM decreased plasma MDA-LDL adducts and prevented the accumulation of plaque MDA- and IsoLG-lysyl adducts in Ldlr mice. In addition, PPM increased the net cholesterol efflux capacity of HDL from Ldlr mice and prevented both the in vitro impairment of HDL net cholesterol efflux capacity and apoAI crosslinking by MPO generated hypochlorous acid. Moreover, PPM decreased features of plaque instability including decreased proinflammatory M1-like macrophages, IL-1β expression, myeloperoxidase, apoptosis, and necrotic core. In contrast, PPM increased M2-like macrophages, Tregs, fibrous cap thickness, and efferocytosis. Furthermore, PPM reduced inflammatory monocytosis as evidenced by decreased blood Ly6C monocytes and proliferation of bone marrow monocytes and HSPC from Ldlr mice.
PPM has pleotropic atheroprotective effects in a murine model of familial hypercholesterolemia, supporting the therapeutic potential of reactive dicarbonyl scavenging in the treatment of IR and atherosclerotic cardiovascular disease.
氧化应激导致胰岛素抵抗(IR)和动脉粥样硬化的发生。脂质过氧化会产生具有反应性的二羰基化合物,如异莱格醛(IsoLG)和丙二醛(MDA),它们会与血浆/细胞蛋白、磷脂和 DNA 发生共价结合,导致其功能和毒性改变。我们研究了用 5'-O-戊基-吡哆胺(PPM)清除具有反应性的二羰基化合物是否可以预防 LDLr 小鼠 IR 和动脉粥样硬化的发生。
雄性或雌性 LDLr 小鼠喂食西方饮食(WD)16 周,并单独用 PPM 或载体处理。测量斑块程度、二羰基赖氨酸加合物、噬作用、细胞凋亡、巨噬细胞炎症和坏死面积。测量血浆 MDA-LDL 加合物以及 PPM 在体内和体外对 HDL 降低巨噬细胞胆固醇能力的影响。还检测了血液 Ly6C 单核细胞以及骨髓 CD11b+单核细胞和 CD34+造血干细胞和祖细胞(HSPC)的 exvivo5-乙炔基-2'-脱氧尿苷(EdU)掺入情况。通过测量空腹血糖/胰岛素水平以及胰岛素/葡萄糖耐量试验来评估 IR。
PPM 使雄性和雌性 LDLr 小鼠的近端主动脉粥样硬化分别减少了 48%和 46%。PPM 还降低了雄性 LDLr 小鼠的 IR 和肝脂肪及炎症。重要的是,PPM 降低了血浆 MDA-LDL 加合物,并防止了 LDLr 小鼠中斑块 MDA 和 IsoLG 赖氨酸加合物的积累。此外,PPM 增加了 LDLr 小鼠 HDL 的净胆固醇流出能力,并防止了 MPO 生成的次氯酸引起的 HDL 净胆固醇流出能力和 apoAI 交联的体外损害。此外,PPM 降低了斑块不稳定性的特征,包括减少促炎 M1 样巨噬细胞、IL-1β 表达、髓过氧化物酶、细胞凋亡和坏死核心。相比之下,PPM 增加了 M2 样巨噬细胞、Tregs、纤维帽厚度和噬作用。此外,PPM 减少了 LDLr 小鼠的炎性单核细胞,表现为血液 Ly6C 单核细胞减少以及骨髓单核细胞和 HSPC 的增殖减少。
PPM 在家族性高胆固醇血症的小鼠模型中具有多种抗动脉粥样硬化作用,支持用清除具有反应性的二羰基化合物治疗 IR 和动脉粥样硬化性心血管疾病的治疗潜力。
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