Nucleoporin93 (Nup93) Limits Yap Activity to Prevent Endothelial Cell Senescence

Tung D Nguyen, Mihir K Rao, Shaiva P Dhyani, Justin M Banks, Michael A Winek, Julka Michalkiewicz, Monica Y Lee
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Abstract

Endothelial cells (ECs) form the innermost lining of the vasculature and serve a pivotal role in preventing age-related vascular disease. Endothelial health relies on the proper nucleocytoplasmic shuttling of transcription factors via nuclear pore complexes (NPCs). Emerging studies report NPC degradation with natural aging, suggesting impaired nucleocytoplasmic transport in age-related EC dysfunction. We herein identify nucleoporin93 (Nup93), a crucial structural NPC protein, as an indispensable player for vascular protection. Endothelial Nup93 protein levels are significantly reduced in the vasculature of aged mice, paralleling observations of Nup93 loss when using in vitro models of endothelial aging. Mechanistically, we find that loss of Nup93 impairs NPC transport, leading to the nuclear accumulation of Yap and downstream inflammation. Collectively, our findings indicate maintenance of endothelial Nup93 as a key determinant of EC health, where aging targets endothelial Nup93 levels to impair NPC function as a novel mechanism for EC senescence and vascular aging.
核孔蛋白93 (Nup93)限制Yap活性防止内皮细胞衰老
内皮细胞(ECs)形成血管的最内层,在预防与年龄相关的血管疾病中起着关键作用。内皮细胞的健康依赖于转录因子通过核孔复合物(NPCs)在核胞质中进行适当的穿梭。新研究报告了NPC随着自然衰老而退化,表明核细胞质运输受损与年龄相关的EC功能障碍有关。我们在此发现核孔蛋白93 (Nup93)是一种重要的NPC结构蛋白,在血管保护中扮演着不可或缺的角色。衰老小鼠血管中内皮细胞Nup93蛋白水平显著降低,这与体外内皮细胞衰老模型中Nup93缺失的观察结果相似。在机制上,我们发现Nup93的缺失会损害NPC的运输,导致Yap的核积聚和下游炎症。总之,我们的研究结果表明,内皮细胞Nup93的维持是EC健康的关键决定因素,而衰老目标是内皮细胞Nup93水平,从而损害NPC功能,这是EC衰老和血管衰老的新机制。
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