外泌体衍生的无饥饿素通过抑制内皮细胞自噬减轻动脉损伤后再狭窄
Intervention of Asprosin Attenuates Oxidative Stress and Neointima Formation in Vascular Injury.
机构信息
Key Laboratory of Targeted Intervention of Cardiovascular Disease, Collaborative Innovation Center for Cardiovascular Disease Translational Medicine, and Department of Physiology, Nanjing Medical University, Nanjing, People's Republic of China.
Department of Pathophysiology, Nanjing Medical University, Nanjing, People's Republic China.
出版信息
Antioxid Redox Signal. 2024 Sep;41(7-9):488-504. doi: 10.1089/ars.2023.0383. Epub 2024 Jul 10.
Asprosin, a newly discovered hormone, is linked to insulin resistance. This study shows the roles of asprosin in vascular smooth muscle cell (VSMC) proliferation, migration, oxidative stress, and neointima formation of vascular injury. Mouse aortic VSMCs were cultured, and platelet-derived growth factor-BB (PDGF-BB) was used to induce oxidative stress, proliferation, and migration in VSMCs. Vascular injury was induced by repeatedly moving a guidewire in the lumen of the carotid artery in mice. Asprosin overexpression promoted VSMC oxidative stress, proliferation, and migration, which were attenuated by toll-like receptor 4 (TLR4) knockdown, antioxidant (N-Acetylcysteine, NAC), NADPH oxidase 1 (NOX1) inhibitor ML171, or NOX2 inhibitor GSK2795039. Asprosin overexpression increased NOX1/2 expressions, whereas asprosin knockdown increased heme oxygenase-1 (HO-1) and NADPH quinone oxidoreductase-1 (NQO-1) expressions. Asprosin inhibited nuclear factor E2-related factor 2 (Nrf2) nuclear translocation. Nrf2 activator sulforaphane increased HO-1 and NQO-1 expressions and prevented asprosin-induced NOX1/2 upregulation, oxidative stress, proliferation, and migration. Exogenous asprosin protein had similar roles to asprosin overexpression. PDGF-BB increased asprosin expressions. PDGF-BB-induced oxidative stress, proliferation, and migration were enhanced by Nrf2 inhibitor ML385 but attenuated by asprosin knockdown. Vascular injury increased asprosin expression. Local asprosin knockdown in the injured carotid artery promoted HO-1 and NQO-1 expressions but attenuated the NOX1 and NOX2 upregulation, oxidative stress, neointima formation, and vascular remodeling in mice. Asprosin promotes oxidative stress, proliferation, and migration of VSMCs TLR4-Nrf2-mediated redox imbalance. Inhibition of asprosin expression attenuates VSMC proliferation and migration, oxidative stress, and neointima formation in the injured artery. Asprosin might be a promising therapeutic target for vascular injury. 41, 488-504.
胰高血糖素原/神经肽 Y 前体衍生肽(Asprosin),一种新发现的激素,与胰岛素抵抗有关。本研究探讨了 Asprosin 在血管平滑肌细胞(VSMC)增殖、迁移、氧化应激和血管损伤新生内膜形成中的作用。培养小鼠主动脉 VSMC,用血小板衍生生长因子-BB(PDGF-BB)诱导 VSMC 氧化应激、增殖和迁移。通过在小鼠颈总动脉管腔内反复移动导丝诱导血管损伤。Asprosin 过表达促进 VSMC 氧化应激、增殖和迁移,TLR4 敲低、抗氧化剂(N-乙酰半胱氨酸,NAC)、NADPH 氧化酶 1(NOX1)抑制剂 ML171 或 NOX2 抑制剂 GSK2795039 可减轻这种作用。Asprosin 过表达增加了 NOX1/2 的表达,而 Asprosin 敲低增加了血红素加氧酶-1(HO-1)和 NADPH 醌氧化还原酶-1(NQO-1)的表达。Asprosin 抑制核因子 E2 相关因子 2(Nrf2)核转位。Nrf2 激活剂萝卜硫素增加了 HO-1 和 NQO-1 的表达,并防止了 Asprosin 诱导的 NOX1/2 上调、氧化应激、增殖和迁移。外源性 Asprosin 蛋白具有与 Asprosin 过表达相似的作用。PDGF-BB 增加了 Asprosin 的表达。Nrf2 抑制剂 ML385 增强了 PDGF-BB 诱导的氧化应激、增殖和迁移,但 Asprosin 敲低则减弱了这种作用。血管损伤增加了 Asprosin 的表达。损伤颈动脉局部 Asprosin 敲低促进了 HO-1 和 NQO-1 的表达,但减轻了小鼠血管中 NOX1 和 NOX2 的上调、氧化应激、新生内膜形成和血管重塑。Asprosin 促进血管平滑肌细胞的氧化应激、增殖和迁移,TLR4-Nrf2 介导的氧化还原失衡。抑制 Asprosin 表达可减轻损伤动脉中 VSMC 的增殖和迁移、氧化应激和新生内膜形成。Asprosin 可能是血管损伤的一个有前途的治疗靶点。 41, 488-504.
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