氧化磷脂 PGPC 通过促进 FABP3 介导的内皮细胞铁死亡来损害内皮功能。
The oxidized phospholipid PGPC impairs endothelial function by promoting endothelial cell ferroptosis via FABP3.
机构信息
Division of Cardiac Surgery, Cardiovascular Diseases Institute, The First Affiliated Hospital, Sun Yat-sen University, Guangzhou, China; National-Guangdong Joint Engineering Laboratory for Diagnosis and Treatment of Vascular Diseases, NHC Key Laboratory of Assisted Circulation and Vascular Diseases (Sun Yat-sen University), Key Laboratory of Assisted Circulation and Vascular Diseases, Chinese Academy of Medical Sciences, Guangdong Provincial Engineering and Technology Center for Diagnosis and Treatment of Vascular Diseases, Guangzhou, China.
National-Guangdong Joint Engineering Laboratory for Diagnosis and Treatment of Vascular Diseases, NHC Key Laboratory of Assisted Circulation and Vascular Diseases (Sun Yat-sen University), Key Laboratory of Assisted Circulation and Vascular Diseases, Chinese Academy of Medical Sciences, Guangdong Provincial Engineering and Technology Center for Diagnosis and Treatment of Vascular Diseases, Guangzhou, China; Division of Hypertension and Vascular Diseases, Department of Cardiology, Cardiovascular Diseases Institute, The First Affiliated Hospital, Sun Yat-sen University, Guangzhou, China.
出版信息
J Lipid Res. 2024 Feb;65(2):100499. doi: 10.1016/j.jlr.2024.100499. Epub 2024 Jan 11.
Ferroptosis is a novel cell death mechanism that is mediated by iron-dependent lipid peroxidation. It may be involved in atherosclerosis development. Products of phospholipid oxidation play a key role in atherosclerosis. 1-palmitoyl-2-glutaroyl-sn-glycero-3-phosphocholine (PGPC) is a phospholipid oxidation product present in atherosclerotic lesions. It remains unclear whether PGPC causes atherosclerosis by inducing endothelial cell ferroptosis. In this study, human umbilical vein endothelial cells (HUVECs) were treated with PGPC. Intracellular levels of ferrous iron, lipid peroxidation, superoxide anions (O), and glutathione were detected, and expression of fatty acid binding protein-3 (FABP3), glutathione peroxidase 4 (GPX4), and CD36 were measured. Additionally, the mitochondrial membrane potential (MMP) was determined. Aortas from C57BL6 mice were isolated for vasodilation testing. Results showed that PGPC increased ferrous iron levels, the production of lipid peroxidation and O, and FABP3 expression. However, PGPC inhibited the expression of GPX4 and glutathione production and destroyed normal MMP. These effects were also blocked by ferrostatin-1, an inhibitor of ferroptosis. FABP3 silencing significantly reversed the effect of PGPC. Furthermore, PGPC stimulated CD36 expression. Conversely, CD36 silencing reversed the effects of PGPC, including PGPC-induced FABP3 expression. Importantly, E06, a direct inhibitor of the oxidized 1-palmitoyl-2-arachidonoyl-phosphatidylcholine IgM natural antibody, inhibited the effects of PGPC. Finally, PGPC impaired endothelium-dependent vasodilation, ferrostatin-1 or FABP3 inhibitors inhibited this impairment. Our data demonstrate that PGPC impairs endothelial function by inducing endothelial cell ferroptosis through the CD36 receptor to increase FABP3 expression. Our findings provide new insights into the mechanisms of atherosclerosis and a therapeutic target for atherosclerosis.
铁死亡是一种新型的细胞死亡机制,由铁依赖性脂质过氧化介导。它可能参与动脉粥样硬化的发展。磷脂氧化产物在动脉粥样硬化中起关键作用。1-棕榈酰基-2-戊二酰基-sn-甘油-3-磷酸胆碱(PGPC)是一种存在于动脉粥样硬化病变中的磷脂氧化产物。目前尚不清楚 PGPC 是否通过诱导内皮细胞铁死亡引起动脉粥样硬化。在这项研究中,用人脐静脉内皮细胞(HUVEC)处理 PGPC。检测细胞内亚铁离子、脂质过氧化、超氧阴离子(O)和谷胱甘肽的水平,并测量脂肪酸结合蛋白 3(FABP3)、谷胱甘肽过氧化物酶 4(GPX4)和 CD36 的表达。此外,还测定了线粒体膜电位(MMP)。分离 C57BL6 小鼠的主动脉进行血管扩张测试。结果表明,PGPC 增加了亚铁离子水平、脂质过氧化和 O 的产生以及 FABP3 的表达。然而,PGPC 抑制了 GPX4 的表达和谷胱甘肽的产生,并破坏了正常的 MMP。这些作用也被铁死亡抑制剂 ferrostatin-1 阻断。FABP3 沉默显著逆转了 PGPC 的作用。此外,PGPC 刺激 CD36 的表达。相反,CD36 沉默逆转了 PGPC 的作用,包括 PGPC 诱导的 FABP3 表达。重要的是,直接抑制 1-棕榈酰基-2-花生四烯酸磷脂酰胆碱 IgM 天然抗体氧化的 E06 抑制了 PGPC 的作用。最后,PGPC 损害了内皮依赖性血管舒张,ferrostatin-1 或 FABP3 抑制剂抑制了这种损害。我们的数据表明,PGPC 通过 CD36 受体诱导内皮细胞铁死亡来增加 FABP3 的表达,从而损害内皮功能。我们的研究结果为动脉粥样硬化的发病机制提供了新的见解,并为动脉粥样硬化提供了一个治疗靶点。
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