Graduate Institute of Medical Sciences, College of Medicine, Taipei Medical University, Taipei, Taiwan.
Biochem Pharmacol. 2012 Oct 1;84(7):914-24. doi: 10.1016/j.bcp.2012.06.030. Epub 2012 Jul 4.
Andrographolide, a novel nuclear factor-κB (NF-κB) inhibitor, is isolated from leaves of Andrographis paniculata. Platelet activation is relevant to a variety of coronary heart diseases. Our recent studies revealed that andrographolide possesses potent antiplatelet activity by activating the endothelial nitric oxide synthase (eNOS)-NO-cyclic GMP pathway. Although platelets are anucleated cells, they also express the transcription factor, NF-κB, that may exert non-genomic functions in platelet activation. Therefore, we further investigated the inhibitory roles of andrographolide in NF-κB-mediated events in platelets. In this study, NF-κB signaling events, including IKKβ phosphorylation, IκBα degradation, and p65 phosphorylation, were time-dependently activated by collagen in human platelets, and these signaling events were attenuated by andrographolide (35 and 75 μM). ODQ and KT5823, respective inhibitors of guanylate cyclase and cyclic GMP-dependent kinase (PKG), strongly reversed andrographolide-mediated inhibition of platelet aggregation, relative [Ca(2+)]i mobilization, and IKKβ, and p65 phosphorylation. In addition, SB203580 (an inhibitor of p38 MAPK), but not PD98059 (an inhibitor of ERKs), markedly abolished IKKβ and p65 phosphorylation. SB203580, NAC (a free-radical scavenger), and BAY11-7082 (an inhibitor of NF-κB) all diminished ERK2 phosphorylation, whereas PD98059, BAY11-7082, and NAC had no effects on p38 MAPK phosphorylation. Furthermore, SB203580, but not BAY11-7082 or PD98059, reduced collagen-induced hydroxyl radical ((·)HO) formation. KT5823 also markedly reversed andrographolide-mediated inhibition of p38 MAPK and ERK2 phosphorylation, and hydroxyl radical formation in platelets. In conclusion, this study demonstrated that andrographolide may involve an increase in cyclic GMP/PKG, followed by inhibition of the p38 MAPK/(·)HO-NF-κB-ERK2 cascade in activated platelets. Therefore, andrographolide may have a high therapeutic potential to treat thromboembolic disorders and may also be considered for treating various inflammatory diseases.
穿心莲内酯是一种从穿心莲属植物叶子中分离得到的新型核因子-κB(NF-κB)抑制剂。血小板激活与多种冠心病有关。我们最近的研究表明,穿心莲内酯通过激活内皮型一氧化氮合酶(eNOS)-NO-cGMP 途径具有强大的抗血小板活性。尽管血小板是无核细胞,但它们也表达转录因子 NF-κB,该因子可能在血小板激活中发挥非基因组功能。因此,我们进一步研究了穿心莲内酯在 NF-κB 介导的血小板事件中的抑制作用。在这项研究中,胶原可时间依赖性地激活人血小板中的 NF-κB 信号事件,包括 IKKβ磷酸化、IκBα降解和 p65磷酸化,而穿心莲内酯(35 和 75μM)可减弱这些信号事件。ODQ 和 KT5823 分别为鸟苷酸环化酶和环磷酸鸟苷依赖性激酶(PKG)的抑制剂,可强烈逆转穿心莲内酯介导的血小板聚集、相对[Ca2+]i 动员和 IKKβ及 p65磷酸化的抑制作用。此外,SB203580(p38 MAPK 的抑制剂)而非 PD98059(ERK 的抑制剂)可显著消除 IKKβ和 p65磷酸化。SB203580、NAC(自由基清除剂)和 BAY11-7082(NF-κB 抑制剂)均减弱 ERK2 磷酸化,而 PD98059、BAY11-7082 和 NAC 对 p38 MAPK 磷酸化无影响。此外,SB203580 而非 BAY11-7082 或 PD98059 可降低胶原诱导的羟自由基(·HO)形成。KT5823 还显著逆转了穿心莲内酯介导的 p38 MAPK 和 ERK2 磷酸化以及血小板中羟自由基的形成。总之,本研究表明,穿心莲内酯可能通过增加环鸟苷酸/蛋白激酶 G(PKG),随后抑制激活血小板中的 p38 MAPK/·HO-NF-κB-ERK2 级联反应,从而发挥作用。因此,穿心莲内酯可能具有治疗血栓栓塞性疾病的高治疗潜力,也可考虑用于治疗各种炎症性疾病。
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