CD163+巨噬细胞诱导动脉粥样斑块中的内皮细胞向间质转化

IF 16.5 1区医学 Q1 CARDIAC & CARDIOVASCULAR SYSTEMS

Circulation research Pub Date : 2024-07-05 Epub Date: 2024-06-11 DOI:10.1161/CIRCRESAHA.123.324082

Masayuki Mori, Atsushi Sakamoto, Rika Kawakami, Liang Guo, Lotte Slenders, Jose Verdezoto Mosquera, Saikat Kumar B Ghosh, Marian Wesseling, Tatsuya Shiraki, Arielle Bellissard, Palak Shah, Craig C Weinkauf, Takao Konishi, Yu Sato, Anne Cornelissen, Kenji Kawai, Hiroyuki Jinnouchi, Weili Xu, Aimee E Vozenilek, Desiree Williams, Takamasa Tanaka, Teruo Sekimoto, Michael C Kelly, Raquel Fernandez, Alyssa Grogan, A J Coslet, Alisa Fedotova, Anjali Kurse, Michal Mokry, Maria E Romero, Frank D Kolodgie, Gerard Pasterkamp, Clint L Miller, Renu Virmani, Aloke V Finn

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引用次数: 0

摘要

背景：越来越多的人认识到动脉粥样硬化中存在细胞表型转换。然而，我们对这种细胞转化的确切刺激因素及其对人类动脉粥样硬化的意义的认识仍在不断发展。斑块内出血被认为是斑块进展的一个主要因素，部分原因是刺激了 CD163+ 巨噬细胞的涌入。在此，我们探讨了 CD163 巨噬细胞通过在纤维帽内诱导促凋亡的内皮细胞向间质转化（EndMT）而导致斑块进展的假设。使用易发生粥样硬化的载脂蛋白E-/-小鼠和载脂蛋白E-/-/CD163-/-小鼠进行体内研究。体外实验使用人外周血单核细胞诱导的巨噬细胞和人主动脉内皮细胞：结果：在 107 例急性冠状动脉斑块破裂病例中，55% 的病理证据显示非斑块破裂血管/病变斑块内出血。在非斑块内出血病变中观察到纤维帽更薄、CD163+巨噬细胞聚集更多，以及纤维帽中CD31/FSP-1（成纤维细胞特异性蛋白-1）双阳性细胞和TUNEL阳性细胞数量更多。用暴露于血红蛋白/aptoglobin的巨噬细胞上清液培养的人主动脉内皮细胞显示，间质标志蛋白（transgelin和FSP-1）增加，而内皮标志蛋白（VE-cadherin和CD31）减少，这表明EndMT诱导。CD163+ 巨噬细胞释放的促炎细胞因子激活了 NF-κB（核因子卡巴 β）信号传导，直接调节了 EndMT 诱导过程中的关键转录因子 Snail 的表达。对裂解的 Caspase 3 进行的 Western 印迹分析和对人主动脉内皮细胞进行的芯片分析表明，在 CD163+ 巨噬细胞诱导 EndMT 的过程中，细胞凋亡受到刺激。此外，动脉粥样硬化小鼠的 CD163 缺失表明，CD163 是 EndMT 和斑块进展所必需的。通过对人类颈动脉内膜切除病变进行单细胞 RNA 测序，检测到了 EndMT 群体，其凋亡相关基因显著上调：结论：CD163+巨噬细胞可诱发EndMT，EndMT可通过纤维帽变薄促进斑块进展。

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CD163⁺ Macrophages Induce Endothelial-to-Mesenchymal Transition in Atheroma.

Background: Cell phenotype switching is increasingly being recognized in atherosclerosis. However, our understanding of the exact stimuli for such cellular transformations and their significance for human atherosclerosis is still evolving. Intraplaque hemorrhage is thought to be a major contributor to plaque progression in part by stimulating the influx of CD163⁺ macrophages. Here, we explored the hypothesis that CD163⁺ macrophages cause plaque progression through the induction of proapoptotic endothelial-to-mesenchymal transition (EndMT) within the fibrous cap.

Methods: Human coronary artery sections from CVPath's autopsy registry were selected for pathological analysis. Athero-prone ApoE^-/- and ApoE^-/-/CD163^-/- mice were used for in vivo studies. Human peripheral blood mononuclear cell-induced macrophages and human aortic endothelial cells were used for in vitro experiments.

Results: In 107 lesions with acute coronary plaque rupture, 55% had pathological evidence of intraplaque hemorrhage in nonculprit vessels/lesions. Thinner fibrous cap, greater CD163⁺ macrophage accumulation, and a larger number of CD31/FSP-1 (fibroblast specific protein-1) double-positive cells and TUNEL (terminal deoxynucleotidyl transferase-dUTP nick end labeling) positive cells in the fibrous cap were observed in nonculprit intraplaque hemorrhage lesions, as well as in culprit rupture sections versus nonculprit fibroatheroma sections. Human aortic endothelial cells cultured with supernatants from hemoglobin/haptoglobin-exposed macrophages showed that increased mesenchymal marker proteins (transgelin and FSP-1) while endothelial markers (VE-cadherin and CD31) were reduced, suggesting EndMT induction. Activation of NF-κB (nuclear factor kappa β) signaling by proinflammatory cytokines released from CD163⁺ macrophages directly regulated the expression of Snail, a critical transcription factor during EndMT induction. Western blot analysis for cleaved caspase-3 and microarray analysis of human aortic endothelial cells indicated that apoptosis was stimulated during CD163⁺ macrophage-induced EndMT. Additionally, CD163 deletion in athero-prone mice suggested that CD163 is required for EndMT and plaque progression. Using single-cell RNA sequencing from human carotid endarterectomy lesions, a population of EndMT was detected, which demonstrated significant upregulation of apoptosis-related genes.

Conclusions: CD163⁺ macrophages provoke EndMT, which may promote plaque progression through fibrous cap thinning.

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来源期刊

Circulation research 医学-外周血管病

CiteScore

29.60

自引率

2.00%

发文量

535

审稿时长

3-6 weeks

期刊介绍： Circulation Research is a peer-reviewed journal that serves as a forum for the highest quality research in basic cardiovascular biology. The journal publishes studies that utilize state-of-the-art approaches to investigate mechanisms of human disease, as well as translational and clinical research that provide fundamental insights into the basis of disease and the mechanism of therapies. Circulation Research has a broad audience that includes clinical and academic cardiologists, basic cardiovascular scientists, physiologists, cellular and molecular biologists, and cardiovascular pharmacologists. The journal aims to advance the understanding of cardiovascular biology and disease by disseminating cutting-edge research to these diverse communities. In terms of indexing, Circulation Research is included in several prominent scientific databases, including BIOSIS, CAB Abstracts, Chemical Abstracts, Current Contents, EMBASE, and MEDLINE. This ensures that the journal's articles are easily discoverable and accessible to researchers in the field. Overall, Circulation Research is a reputable publication that attracts high-quality research and provides a platform for the dissemination of important findings in basic cardiovascular biology and its translational and clinical applications.