人类动脉粥样硬化斑块转录组学发现内皮 beta-2 spectrin 是斑块微血管渗漏表型的潜在调节因子。

IF 9.2 1区 医学 Q1 PERIPHERAL VASCULAR DISEASE Angiogenesis Pub Date : 2024-05-23 DOI:10.1007/s10456-024-09921-z
Timo Rademakers, Marco Manca, Han Jin, Tanguy Orban, Ljubica Matic Perisic, Hubertus J. M. Frissen, Frank Rühle, Petra Hautvast, Jos van Rijssel, Kim van Kuijk, Barend M. E. Mees, Carine J. Peutz-Kootstra, Sylvia Heeneman, Mat J. A. P. Daemen, Gerard Pasterkamp, Monika Stoll, Marc A. M. J. van Zandvoort, Ulf Hedin, Franck Dequiedt, Jaap D. van Buul, Judith C. Sluimer, Erik A. L. Biessen
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引用次数: 0

摘要

动脉粥样硬化斑块血管的存在是斑块不稳定的关键因素。这可能归因于这些微血管的渗漏表型,尽管这一观点还缺乏直接证据。在这项研究中,我们研究了稳定斑块和出血斑块的分子和细胞模式,以确定斑块内血管功能障碍的新驱动因素。从人类动脉粥样硬化病变队列的转录组数据中,我们重建了一个共表达网络,确定了一个与斑块微血管密度和炎症密切相关且具有选择性的基因模块。Spectrin Beta Non-Erythrocytic 1(sptbn1)被确定为该模块的中心枢纽之一(与zeb1和dock1并列),并因其主要的内皮表达而被选作进一步研究的对象。在体外,沉默 sptbn1 会增强白细胞的迁移和血管的通透性,其特征是病灶粘连的数量增加和交界处 VE-cadherin 的减少。在体内,斑马鱼体内敲除 sptbn1 会影响尾静脉丛的发育。在体外和人体血管中,基质硬度的增加与内皮细胞中 sptbn1 的下调有关。研究发现,斑块 SPTBN1 mRNA 和蛋白的表达与斑块内出血和随访期间未来心血管疾病(CVD)事件的增加有关。总之,我们发现 SPTBN1 是斑块血管化相关基因程序的中心枢纽基因。SPTBN1 在体外受基质硬度的调节,而沉默则会阻碍血管在体内的发育,并损害体外的屏障功能。总之,SPTBN1 被确定为动脉粥样硬化斑块微血管渗漏表型的一个新的潜在调节因子。
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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Human atherosclerotic plaque transcriptomics reveals endothelial beta-2 spectrin as a potential regulator a leaky plaque microvasculature phenotype

The presence of atherosclerotic plaque vessels is a critical factor in plaque destabilization. This may be attributable to the leaky phenotype of these microvessels, although direct proof for this notion is lacking. In this study, we investigated molecular and cellular patterns of stable and hemorrhaged human plaque to identify novel drivers of intraplaque vessel dysfunction. From transcriptome data of a human atherosclerotic lesion cohort, we reconstructed a co-expression network, identifying a gene module strongly and selectively correlated with both plaque microvascular density and inflammation. Spectrin Beta Non-Erythrocytic 1 (sptbn1) was identified as one of the central hubs of this module (along with zeb1 and dock1) and was selected for further study based on its predominant endothelial expression. Silencing of sptbn1 enhanced leukocyte transmigration and vascular permeability in vitro, characterized by an increased number of focal adhesions and reduced junctional VE-cadherin. In vivo, sptbn1 knockdown in zebrafish impaired the development of the caudal vein plexus. Mechanistically, increased substrate stiffness was associated with sptbn1 downregulation in endothelial cells in vitro and in human vessels. Plaque SPTBN1 mRNA and protein expression were found to correlate with an enhanced presence of intraplaque hemorrhage and future cardiovascular disease (CVD) events during follow-up. In conclusion, we identify SPTBN1 as a central hub gene in a gene program correlating with plaque vascularisation. SPTBN1 was regulated by substrate stiffness in vitro while silencing blocked vascular development in vivo, and compromised barrier function in vitro. Together, SPTBN1 is identified as a new potential regulator of the leaky phenotype of atherosclerotic plaque microvessels.

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来源期刊
Angiogenesis
Angiogenesis PERIPHERAL VASCULAR DISEASE-
CiteScore
21.90
自引率
8.20%
发文量
37
审稿时长
6-12 weeks
期刊介绍: Angiogenesis, a renowned international journal, seeks to publish high-quality original articles and reviews on the cellular and molecular mechanisms governing angiogenesis in both normal and pathological conditions. By serving as a primary platform for swift communication within the field of angiogenesis research, this multidisciplinary journal showcases pioneering experimental studies utilizing molecular techniques, in vitro methods, animal models, and clinical investigations into angiogenic diseases. Furthermore, Angiogenesis sheds light on cutting-edge therapeutic strategies for promoting or inhibiting angiogenesis, while also highlighting fresh markers and techniques for disease diagnosis and prognosis.
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