DYRK1B inhibition exerts senolytic effects on endothelial cells and rescues endothelial dysfunctions

IF 5.3 3区 医学 Q2 CELL BIOLOGY
Francesca M. Pramotton , Asra Abukar , Chantelle Hudson , James Dunbar , Andrew Potterton , Simone Tonnicchia , Andrea Taddei , Edoardo Mazza , Costanza Giampietro
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引用次数: 1

Abstract

Aging is the major risk factor for chronic disease development. Cellular senescence is a key mechanism that triggers or contributes to age-related phenotypes and pathologies. The endothelium, a single layer of cells lining the inner surface of a blood vessel, is a critical interface between blood and all tissues. Many studies report a link between endothelial cell senescence, inflammation, and diabetic vascular diseases. Here we identify, using combined advanced AI and machine learning, the Dual Specificity Tyrosine Phosphorylation Regulated Kinase 1B (DYRK1B) protein as a possible senolytic target for senescent endothelial cells. We demonstrate that upon induction of senescence in vitro DYRK1B expression is increased in endothelial cells and localized at adherens junctions where it impairs their proper organization and functions. DYRK1B knock-down or inhibition restores endothelial barrier properties and collective behavior. DYRK1B is therefore a possible target to counteract diabetes-associated vascular diseases linked to endothelial cell senescence.

抑制DYRK1B对内皮细胞具有抗衰老作用,可挽救内皮功能障碍
衰老是慢性疾病发展的主要危险因素。细胞衰老是触发或促成年龄相关表型和病理的关键机制。内皮是血管内表面的单层细胞,是血液和所有组织之间的关键界面。许多研究报告内皮细胞衰老、炎症和糖尿病血管疾病之间存在联系。在这里,我们使用先进的人工智能和机器学习相结合,确定了双特异性酪氨酸磷酸化调节激酶1B (DYRK1B)蛋白作为衰老内皮细胞的可能的衰老靶点。我们证明,在体外诱导衰老后,内皮细胞中的DYRK1B表达增加,并定位于粘附连接,从而损害其正常组织和功能。DYRK1B敲除或抑制可恢复内皮屏障特性和集体行为。因此,DYRK1B可能是对抗与内皮细胞衰老相关的糖尿病相关血管疾病的靶点。
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来源期刊
CiteScore
11.10
自引率
1.90%
发文量
79
审稿时长
32 days
期刊介绍: Mechanisms of Ageing and Development is a multidisciplinary journal aimed at revealing the molecular, biochemical and biological mechanisms that underlie the processes of aging and development in various species as well as of age-associated diseases. Emphasis is placed on investigations that delineate the contribution of macromolecular damage and cytotoxicity, genetic programs, epigenetics and genetic instability, mitochondrial function, alterations of metabolism and innovative anti-aging approaches. For all of the mentioned studies it is necessary to address the underlying mechanisms. Mechanisms of Ageing and Development publishes original research, review and mini-review articles. The journal also publishes Special Issues that focus on emerging research areas. Special issues may include all types of articles following peered review. Proposals should be sent directly to the Editor-in-Chief.
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