9p21.3 Coronary Artery Disease Risk Locus Drives Vascular Smooth Muscle Cells to an Osteochondrogenic State.

IF 7.4 1区医学 Q1 HEMATOLOGY

Arteriosclerosis, Thrombosis, and Vascular Biology Pub Date : 2025-03-27 DOI:10.1161/ATVBAHA.124.322045

Elsa Salido, Carolina de Medeiros Vieira, José Verdezoto Mosquera, Rohan Zade, Parth Parikh, Shraddha Suryavanshi, Clint L Miller, Valentina Lo Sardo

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引用次数: 0

Abstract

Background: Genome-wide association studies have identified common genetic variants at ≈300 human genomic loci linked to coronary artery disease susceptibility. Among these genomic regions, the most impactful is the 9p21.3 coronary artery disease risk locus, which spans a 60-kb gene desert and encompasses ≈80 SNPs in high linkage disequilibrium. Despite ≈2 decades since its discovery, the role of the 9p21.3 locus in cells of the vasculature remains incompletely resolved.

Methods: We differentiated induced pluripotent stem cells from risk, nonrisk donors at 9p21.3, and isogenic knockouts into vascular smooth muscle cells (VSMCs). We performed single-cell transcriptomic profiling, including coembedding and comparison with publicly available human arterial data sets. We conducted functional characterization using migration and calcification assays and confirmed our findings on induced pluripotent stem cells-VSMCs derived from additional donors. Finally, we used overexpression of ANRIL followed by gene expression analysis.

Results: We demonstrated that induced pluripotent stem cells-VSMCs harboring the 9p21.3 risk haplotype preferentially adopt an osteochondrogenic state and show remarkable similarity to fibrochondrocytes from human artery tissue. The transcriptional profile and functional assessment of migration and calcification capacity across induced pluripotent stem cell-VSMC lines from multiple donors concordantly resemble an osteochondrogenic state. Importantly, we identified numerous transcription factors driving different VSMC state trajectories. Additionally, we prioritized LIMCH1 and CRABP1 as signature genes critical for defining the risk transcriptional program. Finally, overexpression of a short isoform of ANRIL in 9p21.3 knockout cells was sufficient to induce the osteochondrogenic transcriptional signature.

Conclusions: Our study provides new insights into the mechanism of the 9p21.3 risk locus and defines its previously undescribed role in driving a disease-prone transcriptional and functional state in VSMCs concordant with an osteochondrogenic-like state. Our data suggest that the 9p21.3 risk haplotype likely promotes arterial calcification, through altered expression of ANRIL, in a cell type-specific and cell-autonomous manner, providing insight into potential risk assessment and treatment for carriers.

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冠状动脉疾病风险位点驱动血管平滑肌细胞进入骨软骨生成状态。

背景：全基因组关联研究已经确定了约300个与冠状动脉疾病易感性相关的人类基因组位点的常见遗传变异。在这些基因组区域中，影响最大的是9p21.3冠状动脉疾病风险位点，它跨越60 kb的基因沙漠，包含约80个高度连锁不平衡的snp。尽管9p21.3基因座被发现已近20年，但其在血管细胞中的作用仍未完全确定。方法：我们从9p21.3和等基因敲除的危险供体、非危险供体和血管平滑肌细胞（VSMCs）中分化诱导多能干细胞。我们进行了单细胞转录组分析，包括共包埋和与公开可用的人类动脉数据集的比较。我们使用迁移和钙化试验进行了功能表征，并证实了我们在来自其他供体的诱导多能干细胞（vsmc）上的发现。最后，我们使用过表达ANRIL，然后进行基因表达分析。结果：我们证明了9p21.3风险单倍型诱导多能干细胞- vsmcs优先采用骨软骨形成状态，并与人类动脉组织的纤维软骨细胞具有显著的相似性。来自多个供体的诱导多能干细胞- vsmc细胞系的迁移和钙化能力的转录谱和功能评估一致类似于骨软骨形成状态。重要的是，我们发现了许多驱动不同VSMC状态轨迹的转录因子。此外，我们将LIMCH1和CRABP1作为确定风险转录程序的关键特征基因。最后，在9p21.3敲除细胞中，ANRIL短亚型的过表达足以诱导骨软骨生成的转录特征。结论：我们的研究为9p21.3风险位点的机制提供了新的见解，并定义了其先前未描述的在驱动VSMCs中与骨软骨生成样状态一致的疾病易感转录和功能状态中的作用。我们的数据表明，9p21.3风险单倍型可能通过改变ANRIL的表达，以细胞类型特异性和细胞自主的方式促进动脉钙化，为携带者的潜在风险评估和治疗提供了见解。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Arteriosclerosis, Thrombosis, and Vascular Biology 医学-外周血管病

CiteScore

15.60

自引率

2.30%

发文量

337

审稿时长

2-4 weeks

期刊介绍： The journal "Arteriosclerosis, Thrombosis, and Vascular Biology" (ATVB) is a scientific publication that focuses on the fields of vascular biology, atherosclerosis, and thrombosis. It is a peer-reviewed journal that publishes original research articles, reviews, and other scholarly content related to these areas. The journal is published by the American Heart Association (AHA) and the American Stroke Association (ASA). The journal was published bi-monthly until January 1992, after which it transitioned to a monthly publication schedule. The journal is aimed at a professional audience, including academic cardiologists, vascular biologists, physiologists, pharmacologists and hematologists.