Graduate School of Inner Mongolia Medical University, Inner Mongolia Medical University, Hohhot, 010110, PR China; College of Basic Medicine, Inner Mongolia Medical University, Hohhot, 010110, PR China.
Medical Experiments Center, Inner Mongolia Medical University, Hohhot, 010110, PR China.
Biochem Biophys Res Commun. 2024 Sep 17;725:150236. doi: 10.1016/j.bbrc.2024.150236. Epub 2024 Jun 6.
Macrophage-derived foam cell formation is a hallmark of atherosclerosis and is retained during plaque formation. Strategies to inhibit the accumulation of these cells hold promise as viable options for treating atherosclerosis. Plexin D1 (PLXND1), a member of the Plexin family, has elevated expression in atherosclerotic plaques and correlates with cell migration; however, its role in macrophages remains unclear. We hypothesize that the guidance receptor PLXND1 negatively regulating macrophage mobility to promote the progression of atherosclerosis.
We utilized a mouse model of atherosclerosis based on a high-fat diet and an ox-LDL- induced foam cell model to assess PLXND1 levels and their impact on cell migration. Through western blotting, Transwell assays, and immunofluorescence staining, we explored the potential mechanism by which PLXND1 mediates foam cell motility in atherosclerosis.
Our study identifies a critical role for PLXND1 in atherosclerosis plaques and in a low-migration capacity foam cell model induced by ox-LDL. In the aortic sinus plaques of ApoE mice, immunofluorescence staining revealed significant upregulation of PLXND1 and Sema3E, with colocalization in macrophages. In macrophages treated with ox-LDL, increased expression of PLXND1 led to reduced pseudopodia formation and decreased migratory capacity. PLXND1 is involved in regulating macrophage migration by modulating the phosphorylation levels of FAK/Paxillin and downstream CDC42/PAK. Additionally, FAK inhibitors counteract the ox-LDL-induced migration suppression by modulating the phosphorylation states of FAK, Paxillin and their downstream effectors CDC42 and PAK.
Our findings indicate that PLXND1 plays a role in regulating macrophage migration by modulating the phosphorylation levels of FAK/Paxillin and downstream CDC42/PAK to promoting atherosclerosis.
巨噬细胞源性泡沫细胞的形成是动脉粥样硬化的一个标志,并且在斑块形成过程中仍然存在。抑制这些细胞积累的策略作为治疗动脉粥样硬化的可行选择具有很大的潜力。Plexin D1(PLXND1)是 Plexin 家族的一员,在动脉粥样硬化斑块中表达升高,并与细胞迁移相关;然而,其在巨噬细胞中的作用尚不清楚。我们假设,导向受体 PLXND1 通过负调控巨噬细胞迁移来促进动脉粥样硬化的进展。
我们利用高脂肪饮食和 ox-LDL 诱导的泡沫细胞模型的动脉粥样硬化小鼠模型来评估 PLXND1 水平及其对细胞迁移的影响。通过 Western blot、Transwell 测定和免疫荧光染色,我们探讨了 PLXND1 介导动脉粥样硬化中泡沫细胞运动的潜在机制。
我们的研究确定了 PLXND1 在动脉粥样硬化斑块和 ox-LDL 诱导的低迁移能力泡沫细胞模型中的关键作用。在 ApoE 小鼠的主动脉窦斑块中,免疫荧光染色显示 PLXND1 和 Sema3E 显著上调,并与巨噬细胞共定位。在 ox-LDL 处理的巨噬细胞中,PLXND1 的表达增加导致伪足形成减少和迁移能力降低。PLXND1 通过调节 FAK/Paxillin 及其下游 CDC42/PAK 的磷酸化水平来参与调节巨噬细胞迁移。此外,FAK 抑制剂通过调节 FAK、Paxillin 及其下游效应物 CDC42 和 PAK 的磷酸化状态来拮抗 ox-LDL 诱导的迁移抑制。
我们的研究结果表明,PLXND1 通过调节 FAK/Paxillin 和下游 CDC42/PAK 的磷酸化水平来调节巨噬细胞迁移,从而促进动脉粥样硬化。
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