三七总皂苷通过 Piezo1 信号通路缓解低切诱导的内皮炎症和血栓形成。
Effects of Panax notoginseng saponins on alleviating low shear induced endothelial inflammation and thrombosis via Piezo1 signalling.
机构信息
Institute of Chinese Materia Medica, China Academy of Chinese Medical Sciences, Beijing, China.
Institute of Chinese Materia Medica, China Academy of Chinese Medical Sciences, Beijing, China.
出版信息
J Ethnopharmacol. 2024 Dec 5;335:118639. doi: 10.1016/j.jep.2024.118639. Epub 2024 Jul 30.
ETHNOPHARMACOLOGICAL RELEVANCE
Panax notoginseng saponins (PNS) are the major effective components of Panax notoginseng (burk) F.H.Chen which is one of the classic promoting blood circulation herbs in traditional Chinese medicine. PNS is widely used in China for the treatment of cerebral ischemic stroke. Pathological low shear stress is a causal factor in endothelial inflammation and thrombosis. However, the mechanism of PNS against low shear related endothelial inflammation is still unclear.
AIM TO THE STUDY
This study aims to investigate the effects of PNS against endothelial inflammation induced by low shear stress and to explore the underlying mechanical and biological mechanisms.
MATERIALS AND METHODS
Mouse model of carotid partial ligation for inducing low endothelial shear stress was established, the pharmacodynamic effect and mechanism of PNS against endothelial inflammation induced by low shear stress through Piezo1 were explored. Yoda1-evoked Piezo1 activation and expression in human umbilical vein endothelial cells (HUVECs) were determined at static condition. Microfluidic channel systems were used to apply shear stress on HUVECs and Piezo1 siRNA HUVECs to determine PECAM-1, p-YAP and VCAM-1 expression. And platelet rich plasma (PRP) was introduced to low shear treated endothelial cells surface to observe the adhesion and activation by fluorescence imaging and flowcytometry.
RESULTS
PNS attenuated endothelial inflammation and improved blood flow in a reasonable dose response pattern in carotid partial ligation mouse model by influencing Piezo1 and PECAM-1 expression, while suppressing yes-associated protein (YAP) nuclear translocation. We found Piezo1 sensed abnormal shear stress and transduced these mechanical signals by different pathways in HUVECs, and PNS relieved endothelial inflammation induced by low shear stress through Piezo1. We also found Piezo1 signalling has interaction with PECAM-1 under low shear stress, which were involved in platelets adhesion to endothelial cells. Low shear stress increased YAP nuclear translocation and increased VCAM-1 expression in HUVECs which might activate platelets. PNS inhibited low shear induced Piezo1 and PECAM-1 expression and YAP nuclear translocation in HUVECs, furthermore inhibited platelet adhesion and activation on dysfunctional endothelial cells induced by low shear stress.
CONCLUSION
PNS ameliorated endothelial inflammation and thrombosis induced by low shear stress through modulation of the Piezo1 channel, PECAM-1 expression, and YAP nuclear translocation. PNS might serve as a potential therapeutic candidate for ameliorating endothelial inflammation induced by abnormal blood shear stress.
民族药理学相关性
三七总皂苷(PNS)是三七(burk)F.H.Chen 的主要有效成分之一,是中药中经典的活血化瘀药之一。PNS 在中国被广泛用于治疗脑缺血性中风。病理性低切应力是内皮炎症和血栓形成的一个因果因素。然而,PNS 对抗低切相关内皮炎症的机制尚不清楚。
目的
本研究旨在探讨 PNS 对低切应力诱导的内皮炎症的作用,并探讨其潜在的力学和生物学机制。
材料与方法
建立了颈动脉部分结扎诱导内皮低剪切应力的小鼠模型,通过 Piezo1 探讨 PNS 对低剪切诱导内皮炎症的药效学作用及机制。在静态条件下,测定 Yoda1 诱导的人脐静脉内皮细胞(HUVECs)中 Piezo1 的激活和表达。采用微流控通道系统对 HUVECs 和 Piezo1 siRNA HUVECs 施加切应力,测定 PECAM-1、p-YAP 和 VCAM-1 的表达。将富含血小板的血浆(PRP)引入到低切处理的内皮细胞表面,通过荧光成像和流式细胞术观察血小板的黏附和激活。
结果
PNS 通过影响 Piezo1 和 PECAM-1 的表达,以合理的剂量反应模式抑制 YAP 核转位,从而减轻颈动脉部分结扎小鼠模型中的内皮炎症和改善血流。我们发现 Piezo1 在 HUVECs 中感知异常切应力,并通过不同途径传递这些力学信号,PNS 通过 Piezo1 缓解低切应力诱导的内皮炎症。我们还发现 Piezo1 信号在低切应力下与 PECAM-1 相互作用,参与血小板与内皮细胞的黏附。低切应力增加了 HUVECs 中 YAP 的核转位和 VCAM-1 的表达,可能激活血小板。PNS 抑制 HUVECs 中低切诱导的 Piezo1 和 PECAM-1 表达以及 YAP 核转位,进一步抑制低切应力诱导的功能失调内皮细胞上血小板的黏附和激活。
结论
PNS 通过调节 Piezo1 通道、PECAM-1 表达和 YAP 核转位,改善低切应力诱导的内皮炎症和血栓形成。PNS 可能成为一种潜在的治疗候选药物,用于改善异常血流切应力诱导的内皮炎症。
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