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Effects of shinbuto and ninjinto on prostaglandin E2 production in lipopolysaccharide-treated human gingival fibroblasts

机译:信奉和忍者对脂多糖处理的人牙龈成纤维细胞中前列腺素E2产生的影响

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摘要

Previously, we revealed that several kampo medicines used for patients with excess and/or medium patterns (kakkonto (TJ-1), shosaikoto (TJ-9), hangeshashinto (TJ-14), and orento (TJ-120)) reduced prostaglandin (PG)E2 levels using LPS-treated human gingival fibroblasts (HGFs). Recently, we examined other kampo medicines used for patients with the deficiency pattern [bakumondoto (TJ-29), shinbuto (TJ-30), ninjinto (TJ-32), and hochuekkito (TJ-41)] and the herbs comprising shinbuto and ninjinto using the same experimental model. Shinbuto and ninjinto concentration-dependently reduced LPS-induced PGE2 production by HGFs, whereas hochuekkito weakly reduced and bakumondoto did not reduce PGE2 production. Shinbuto and ninjinto did not alter cyclooxygenase (COX) activity or the expression of molecules involved in the arachidonic acid cascade. Therefore, we next examined which herbs compromising shinbuto and ninjinto reduce LPS-induced PGE2 production. Among these herbs, shokyo (Zingiberis Rhizoma) and kankyo (Zingiberis Processum Rhizoma) strongly and concentration-dependently decreased LPS-induced PGE2 production. However, both shokyo and kankyo increased the expression of cytosolic phospholipase (cPL)A2 but did not affect annexin1 or COX-2 expression. These results suggest that shokyo and kankyo suppress cPLA2 activity. We demonstrated that kampo medicines suppress inflammatory responses in patients with the deficiency pattern, and in those with excess or medium patterns. Moreover, kampo medicines that contain shokyo or kankyo are considered to be effective for the treatment of inflammatory diseases.
机译:先前,我们发现,用于具有过多和/或中等模式的患者的多种甘榜药物(kakkonto(TJ-1),shoosaikoto(TJ-9),hangeshashinto(TJ-14)和orento(TJ-120))可降低前列腺素使用LPS处理的人牙龈成纤维细胞(HGF)的(PG)E2水平。最近,我们检查了其他用于患有虚弱模式的患者的药物[bakumondoto(TJ-29),shinbuto(TJ-30),ninjinto(TJ-32)和hochuekkito(TJ-41)],以及包含shinbuto和Ninjinto使用相同的实验模型。 Shinbuto和Ninjinto浓度依赖性地降低了HGF诱导的LPS诱导的PGE2产生,而hochuekkito弱地降低了,bakumondoto没有降低PGE2的产生。 Shinbuto和Ninjinto不会改变环氧合酶(COX)的活性或花生四烯酸级联反应中涉及的分子的表达。因此,我们接下来检查了哪些损害新竹和忍者的草药会降低LPS诱导的PGE2的产生。在这些草药中,shokyo(Zingiberis Rhizoma)和kankyo(Zingiberis Processum Rhizoma)强烈且浓度依赖性地降低LPS诱导的PGE2产生。但是,shokyo和kankyo都增加了胞质磷脂酶(cPL)A2的表达,但不影响Annexin1或COX-2的表达。这些结果表明,shokyo和kankyo抑制cPLA2活性。我们证明,在缺乏模式的患者以及过量或中等模式的患者中,坎波药物会抑制炎症反应。此外,包含松香或kankyo的kampo药物被认为可有效治疗炎性疾病。

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