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Non-genomic effects of the Pregnane X Receptor negatively regulate platelet functions, thrombosis and haemostasis

机译:妊娠X受体的非基因组效应负调节血小板函数,血栓形成和血肿

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The pregnane X receptor (PXR) is a nuclear receptor (NR), involved in the detoxification of xenobiotic compounds. Recently, its presence was reported in the human vasculature and its ligands were proposed to exhibit anti-atherosclerotic effects. Since platelets contribute towards the development of atherosclerosis and possess numerous NRs, we investigated the expression of PXR in platelets along with the ability of its ligands to modulate platelet activation. The expression of PXR in human platelets was confirmed using immunoprecipitation analysis. Treatment with PXR ligands was found to inhibit platelet functions stimulated by a range of agonists, with platelet aggregation, granule secretion, adhesion and spreading on fibrinogen all attenuated along with a reduction in thrombus formation (both in vitro and in vivo). The effects of PXR ligands were observed in a species-specific manner, and the human-specific ligand, SR12813, was observed to attenuate thrombus formation in vivo in humanised PXR transgenic mice. PXR ligand-mediated inhibition of platelet function was found to be associated with the inhibition of Src-family kinases (SFKs). This study identifies acute, non-genomic regulatory effects of PXR ligands on platelet function and thrombus formation. In combination with the emerging anti-atherosclerotic properties of PXR ligands, these anti-thrombotic effects may provide additional cardio-protective benefits.
机译:妊娠X受体(PXR)是核受体(NR),参与异黄素化合物的解毒。最近,在人脉管系统中报道了其存在,并且提出了其配体表现出抗动脉粥样硬化作用。由于血小板有助于动脉粥样硬化的发展并具有许多NRS,我们研究了PXR在血小板中的表达以及其配体调节血小板活化的能力。使用免疫沉淀分析证实了PXR在人血小板中的表达。发现用PXR配体处理抑制由一系列激动剂刺激的血小板函数,具有血小板聚集,颗粒分泌,粘附和在纤维蛋白原上的扩散以及随着血栓形成的还原(体外和体内)的降低。以物种特异性方式观察PXR配体的影响,并且观察到人特异性配体SR12813,以衰减人源化的PXR转基因小鼠体内体内的血栓形成。发现PXR配体介导的血小板功能的抑制与SRC-Family激酶(SFK)的抑制相关。本研究鉴定了PXR配体对血小板函数和血栓形成的急性,非基因组调节作用。结合PXR配体的出现抗动脉粥样硬化特性,这些抗血栓形成效应可以提供额外的心动保护益处。

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