Hypoxia inducible factor 1-alpha in the pathogenesis of abdominal aortic aneurysms in vivo: A narrative review

Q3 Medicine JVS-vascular science Pub Date : 2024-01-01 DOI:10.1016/j.jvssci.2023.100189
Peter James Bruhn MD , Majken Lyhne Jessen MD , Jonas Eiberg MD, PhD , Qasam Ghulam MD, PhD
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Abstract

Abdominal aortic aneurysms (AAAs) are relatively common, primarily among older men, and, in the case of rupture, are associated with high mortality. Although procedure-related morbidity and mortality have improved with the advent of endovascular repair, noninvasive treatment and improved assessment of AAA rupture risk should still be sought. Several cellular pathways seem contributory to the histopathologic changes that drive AAA growth and rupture. Hypoxia inducible factor 1-alpha (HIF-1α) is an oxygen-sensitive protein that accumulates in the cytoplasm under hypoxic conditions and regulates a wide array of downstream effectors to hypoxia. Examining the potential role of HIF-1α in the pathogenesis of AAAs is alluring, because local hypoxia is known to be present in the AAA vessel wall. A systematic scoping review was performed to review the current evidence regarding the role of HIF-1α in AAA disease in vivo. After screening, 17 studies were included in the analysis. Experimental animal studies and human studies show increased HIF-1α activity in AAA tissue compared with healthy aorta and a correlation of HIF-1α activity with key histopathologic features of AAA disease. In vivo HIF-1α inhibition in animals protects against AAA development and growth. One study reveals a positive correlation between HIF-1α–activating genetic polymorphisms and the risk of AAA disease in humans. The main findings suggest a causal role of HIF-1α in the pathogenesis of AAAs in vivo. Further research into the HIF-1α pathway in AAA disease might reveal clinically applicable pharmacologic targets or biomarkers relevant in the treatment and monitoring of AAA disease.

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腹主动脉瘤体内发病机制中的 HIF-1α:叙述性综述
腹主动脉瘤(AAA)比较常见,主要发生在老年男性中,一旦破裂,死亡率很高。虽然随着血管内修复术的出现,与手术相关的发病率和死亡率都有所改善,但仍应寻求无创治疗和改进 AAA 破裂风险评估。导致 AAA 生长和破裂的组织病理学变化似乎有几种细胞途径。缺氧诱导因子 1-α(HIF-1α)是一种氧敏感蛋白,在缺氧条件下会在细胞质中聚集,并调节一系列缺氧下游效应因子。研究 HIF-1α 在 AAA 发病机制中的潜在作用很有吸引力,因为已知 AAA 血管壁存在局部缺氧。我们进行了一项系统性的范围界定审查,以审查有关 HIF-1α 在体内 AAA 疾病中作用的现有证据。经过筛选,17 项研究被纳入分析。实验动物研究和人体研究显示,与健康主动脉相比,AAA 组织中的 HIF-1α 活性增加,而且 HIF-1α 活性与 AAA 疾病的主要组织病理学特征相关。在动物体内抑制 HIF-1α 可防止 AAA 的发生和生长。一项研究揭示了 HIF-1α 激活基因多态性与人类 AAA 疾病风险之间的正相关性。主要研究结果表明,HIF-1α 在 AAA 的体内发病机制中起着因果作用。对AAA疾病中HIF-1α通路的进一步研究可能会发现适用于临床的药物靶点或与治疗和监测AAA疾病相关的生物标志物。
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CiteScore
4.20
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0.00%
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0
审稿时长
28 weeks
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