时空 ATF3 表达决定腹主动脉瘤中 VSMC 的命运。
Spatiotemporal ATF3 Expression Determines VSMC Fate in Abdominal Aortic Aneurysm.
机构信息
Institute of Pediatrics (Y.W., Y. Liu, J.T., X.F., D.L., X.F., C.C., Y.Z., W.H.T.), Guangzhou Women and Children's Medical Centre, Guangzhou Medical University, China.
Department of Vascular Surgery (Q.L.), the Second Affiliated Hospital of Guangzhou Medical University, China.
出版信息
Circ Res. 2024 May 24;134(11):1495-1511. doi: 10.1161/CIRCRESAHA.124.324323. Epub 2024 Apr 30.
BACKGROUND
Abdominal aortic aneurysm (AAA) is a catastrophic disease with little effective therapy, likely due to the limited understanding of the mechanisms underlying AAA development and progression. ATF3 (activating transcription factor 3) has been increasingly recognized as a key regulator of cardiovascular diseases. However, the role of ATF3 in AAA development and progression remains elusive.
METHODS
Genome-wide RNA sequencing analysis was performed on the aorta isolated from saline or Ang II (angiotensin II)-induced AAA mice, and ATF3 was identified as the potential key gene for AAA development. To examine the role of ATF3 in AAA development, vascular smooth muscle cell-specific ATF3 knockdown or overexpressed mice by recombinant adeno-associated virus serotype 9 vectors carrying ATF3, or shRNA-ATF3 with SM22α (smooth muscle protein 22-α) promoter were used in Ang II-induced AAA mice. In human and murine vascular smooth muscle cells, gain or loss of function experiments were performed to investigate the role of ATF3 in vascular smooth muscle cell proliferation and apoptosis.
RESULTS
In both Ang II-induced AAA mice and patients with AAA, the expression of ATF3 was reduced in aneurysm tissues but increased in aortic lesion tissues. The deficiency of ATF3 in vascular smooth muscle cell promoted AAA formation in Ang II-induced AAA mice. PDGFRB (platelet-derived growth factor receptor β) was identified as the target of ATF3, which mediated vascular smooth muscle cell proliferation in response to TNF-alpha (tumor necrosis factor-α) at the early stage of AAA. ATF3 suppressed the mitochondria-dependent apoptosis at the advanced stage by upregulating its direct target BCL2. Our chromatin immunoprecipitation results also demonstrated that the recruitment of NFκB1 and P300/BAF/H3K27ac complex to the ATF3 promoter induces ATF3 transcription via enhancer activation. NFKB1 inhibitor (andrographolide) inhibits the expression of ATF3 by blocking the recruiters NFKB1 and ATF3-enhancer to the ATF3-promoter region, ultimately leading to AAA development.
CONCLUSIONS
Our results demonstrate a previously unrecognized role of ATF3 in AAA development and progression, and ATF3 may serve as a novel therapeutic and prognostic marker for AAA.
背景
腹主动脉瘤(AAA)是一种灾难性疾病,目前治疗方法效果甚微,这可能是由于我们对 AAA 发展和进展的机制了解有限。激活转录因子 3(ATF3)已被越来越多地认为是心血管疾病的关键调节因子。然而,ATF3 在 AAA 发展和进展中的作用仍不清楚。
方法
对盐水或血管紧张素 II(Ang II)诱导的 AAA 小鼠分离的主动脉进行全基因组 RNA 测序分析,鉴定出 ATF3 是 AAA 发展的潜在关键基因。为了研究 ATF3 在 AAA 发展中的作用,使用携带 ATF3 的重组腺相关病毒血清型 9 载体或 SM22α(平滑肌蛋白 22-α)启动子的 shRNA-ATF3 对血管平滑肌细胞特异性 ATF3 敲低或过表达的小鼠进行 Ang II 诱导的 AAA 小鼠实验。在人类和鼠类血管平滑肌细胞中进行增益或缺失功能实验,以研究 ATF3 在血管平滑肌细胞增殖和凋亡中的作用。
结果
在 Ang II 诱导的 AAA 小鼠和 AAA 患者中,AAA 组织中 ATF3 的表达降低,但在主动脉病变组织中升高。血管平滑肌细胞中 ATF3 的缺失促进了 Ang II 诱导的 AAA 小鼠中 AAA 的形成。血小板衍生生长因子受体β(PDGFRB)被鉴定为 ATF3 的靶点,该靶点介导了 TNF-α(肿瘤坏死因子-α)作用下 AAA 早期阶段的血管平滑肌细胞增殖。ATF3 通过上调其直接靶标 BCL2 抑制晚期阶段的线粒体依赖性细胞凋亡。我们的染色质免疫沉淀结果还表明,NFκB1 和 P300/BAF/H3K27ac 复合物募集到 ATF3 启动子上,通过增强子激活诱导 ATF3 转录。NFKB1 抑制剂(穿心莲内酯)通过阻止 NFKB1 和 ATF3-增强子募集到 ATF3 启动子区域来抑制 ATF3 的表达,最终导致 AAA 的发展。
结论
我们的研究结果表明,ATF3 在 AAA 的发展和进展中具有以前未被认识到的作用,ATF3 可能成为 AAA 的一种新的治疗和预后标志物。
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