血液循环细胞PCSK6消融增加动脉粥样硬化负担，但通过激活th17 -平滑肌细胞调节轴提高斑块稳定性

IF 3.5 3区医学 Q2 PHARMACOLOGY & PHARMACY

Vascular pharmacology Pub Date : 2025-03-15 DOI:10.1016/j.vph.2025.107490

Bianca E. Suur , Glykeria Karadimou , Colin J.J.M. Willems , Otto Bergman , Mariette Lengquist , Malin Kronqvist , Roland Baumgartner , Stephen Malin , Anton Gisterå , Göran K. Hansson , Anders Mälarstig , Ulf Hedin , Daniel F.J. Ketelhuth , Ljubica Matic

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引用次数: 0

摘要

蛋白转化酶枯草菌素/酮蛋白（pcsk）与癌症和心血管疾病有关。我们已经证明PCSK6是调节平滑肌细胞（SMC）介导的血管重构的关键蛋白酶，但它也可以通过动脉粥样硬化斑块中的T细胞和巨噬细胞表达。PCSK6是否在血管炎症的背景下调节先天和适应性免疫反应尚不清楚。方法本研究对组成型Pcsk6−/−小鼠进行了详细的免疫分型。采用高胆固醇饮食喂养的Ldlr - / -小鼠进行骨髓移植，研究pcsk6介导的动脉粥样硬化和斑块稳定性的免疫效应。结果与对照组相比，Pcsk6−/−小鼠血浆中化学引诱剂CCL2和CCCL3以及Th17细胞因子il - 17a和IL-17F的水平较高。Pcsk6消融导致脾细胞naïve和效应记忆性CD4+和CD8+细胞数量增加，IL-17 A、IFN-γ和IL-10释放增加，脾细胞增殖增加。缺乏Pcsk6也会影响先天免疫，因为Pcsk6−/−小鼠的巨噬细胞在体外LPS刺激下分泌更多的细胞因子，包括TNF-α、CCL2、IL-6和IL-10，并且更容易摄取oxLDL。与促炎表型一致，与接受Ldlr - / -的对照骨髓相比，Pcsk6 - / -有更高的动脉粥样硬化斑块负担。尽管更大，Pcsk6 - / - Ldlr - / -斑块显示出增加的稳定性特征，包括胶原沉积和SMC的存在，与纤维原性细胞因子IL-17的局部水平显著增加相一致。结论Pcsk6整体消融可激活适应性免疫系统和先天免疫系统。有趣的是，在高脂血症小鼠骨髓中Pcsk6−/−消融揭示了其在动脉粥样硬化发生中的双重作用，激活Th17-SMC调节轴，促进斑块稳定性，尽管增加了动脉粥样硬化负担。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

PCSK6 ablation in blood circulating cells increases atherosclerotic burden, but improves plaque stability by activating Th17-smooth muscle cell modulatory axis

查看原文本刊更多论文

PCSK6 ablation in blood circulating cells increases atherosclerotic burden, but improves plaque stability by activating Th17-smooth muscle cell modulatory axis

Background

Proprotein convertase subtilisins/kexins (PCSKs) have been implicated in cancers and cardiovascular disease. We have shown that PCSK6 is a key protease regulating smooth muscle cell (SMC)-mediated vascular remodeling, but also that it can be expressed by T cells and macrophages in atherosclerotic plaques. Whether PCSK6 regulates innate and adaptive immune responses in the context of vascular inflammation is still unknown.

Methods

In this study, detailed immunophenotyping of constitutive Pcsk6^−/− mice was performed. Bone marrow transplantation into high-cholesterol diet fed Ldlr^−/− mice was used to investigate PCSK6-mediated immune effects in atherogenesis and plaque stability.

Results

Compared to controls, Pcsk6^−/− mice showed higher plasma levels of the chemoattractants CCL2 and CCCL3, and Th17 cytokines IL-17 A and IL-17F. Pcsk6 ablation led to increased naïve and effector-memory CD4+ and CD8+ cell numbers in the spleen, and increased release of IL-17 A, IFN-γ and IL-10 as well as proliferation by spleenocytes in vitro. Lack of Pcsk6 also affected innate immunity as macrophages from Pcsk6^−/− mice secreted more cytokines, including TNF-α, CCL2, IL-6 and IL-10 upon LPS stimulation in vitro, and were more prone to oxLDL uptake. In line with a pro-inflammatory phenotype, Pcsk6^−/−➔Ldlr^−/− transplanted mice presented a higher atherosclerotic plaque burden compared to Ldlr^−/− receiving control bone marrow. Although larger, Pcsk6^−/−➔Ldlr^−/− plaques showed increased stability features, including collagen deposition and SMC presence coinciding with significantly increased local levels of the fibrogenic cytokine IL-17.

Conclusions

Global Pcsk6 ablation leads to the activation of both adaptive and innate immune systems. Interestingly, Pcsk6^−/− ablation in bone marrow of hyperlipidemic mice revealed its dual role in atherogenesis, activating a Th17-SMC modulatory axis that promotes plaque stability, despite increased atherosclerotic burden.

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来源期刊

Vascular pharmacology 医学-药学

CiteScore

6.60

自引率

2.50%

发文量

153

审稿时长

31 days

期刊介绍： Vascular Pharmacology publishes papers, which contains results of all aspects of biology and pharmacology of the vascular system. Papers are encouraged in basic, translational and clinical aspects of Vascular Biology and Pharmacology, utilizing approaches ranging from molecular biology to integrative physiology. All papers are in English. The Journal publishes review articles which include vascular aspects of thrombosis, inflammation, cell signalling, atherosclerosis, and lipid metabolism.