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人类隐静脉暴露于体外动脉血流动力学的空间转录组分析 - 对冠状动脉旁路移植通畅性和静脉移植物疾病的影响。

Spatial Transcriptomic Profiling of Human Saphenous Vein Exposed to Ex Vivo Arterial Haemodynamics-Implications for Coronary Artery Bypass Graft Patency and Vein Graft Disease.

机构信息

Department of Cardiovascular Sciences, University of Leicester, Leicester LE1 7RH, UK.

出版信息

Int J Mol Sci. 2024 Sep 26;25(19):10368. doi: 10.3390/ijms251910368.

Abstract

Vein graft disease is the process by which saphenous vein grafts, utilised for revascularisation during coronary artery bypass graft surgery, undergo an inflammation-driven intimal hyperplasia and accelerated atherosclerosis process in subsequent years after implantation. The role of the arterial circulation, particularly the haemodynamic properties' impact on graft patency, have been investigated but have not to date been explored in depth at the transcriptomic level. We have undertaken the first-in-man spatial transcriptomic analysis of the long saphenous vein in response to ex vivo acute arterial haemodynamic stimulation, utilising a combination of a custom 3D-printed perfusion bioreactor and the 10X Genomics Visium Spatial Gene Expression technology. We identify a total of 413 significant genes (372 upregulated and 41 downregulated) differentially expressed in response to arterial haemodynamic conditions. These genes were associated with pathways including , , , and , among others. These are established pathways involved in the initiation of an early pro-inflammatory response, leukocyte activation and adhesion signalling, tissue remodelling, and cellular differentiation. Utilising unsupervised clustering analysis, we have been able to classify subsets of the expression based on cell type and with spatial resolution. These findings allow for further characterisation of the early saphenous vein graft transcriptional landscape during the earliest stage of implantation that contributes to vein graft disease, in particular validation of pathways and druggable targets that could contribute towards the therapeutic inhibition of processes underpinning vein graft disease.

摘要

静脉移植物疾病是指大隐静脉移植物在冠状动脉旁路移植手术后用于血管重建,在植入后数年经历炎症驱动的内膜增生和加速动脉粥样硬化过程。动脉循环的作用,特别是血流动力学特性对移植物通畅性的影响,已经得到了研究,但迄今为止尚未在转录组水平上进行深入探讨。我们首次对大隐静脉进行了人体空间转录组分析,以响应体外急性动脉血流动力学刺激,结合使用定制的 3D 打印灌注生物反应器和 10X Genomics Visium 空间基因表达技术。我们总共鉴定出 413 个差异表达的显著基因(372 个上调和 41 个下调),这些基因与多种途径相关,包括、、、等。这些是与早期促炎反应、白细胞激活和黏附信号、组织重塑和细胞分化等起始相关的已建立途径。利用无监督聚类分析,我们能够根据细胞类型和空间分辨率对表达的亚群进行分类。这些发现有助于进一步描述在植入早期阶段导致静脉移植物疾病的静脉移植物早期转录谱,特别是验证可能有助于抑制静脉移植物疾病基础过程的途径和可药物治疗的靶点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9117/11476946/f07b6e92f94f/ijms-25-10368-g001.jpg

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