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首页> 外文期刊>The Journal of Allergy and Clinical Immunology >Anti-inflammatory and corticosteroid-enhancing actions of vitamin D in monocytes of patients with steroid-resistant and those with steroid-sensitive asthma
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Anti-inflammatory and corticosteroid-enhancing actions of vitamin D in monocytes of patients with steroid-resistant and those with steroid-sensitive asthma

机译:维生素D对类固醇抵抗性患者和类固醇敏感性哮喘患者的单核细胞中维生素D的消炎和增强作用

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Background Vitamin D is known for its anti-inflammatory effects. Objective Vitamin D regulation of responses in patients with steroid-resistant (SR) versus steroid-sensitive (SS) asthma has not been studied. Methods Peripheral blood cells from 11 patients with SR asthma and 8 patients with SS asthma were preincubated with 1,25-dihydroxyvitamin D (1,25[OH]2D [VitD]), followed by dexamethasone (DEX) treatment and LPS stimulation. LPS-induced phosphorylated p38 mitogen-activated protein kinase (p-p38) in monocytes was examined by means of flow cytometry. Mitogen-activated protein kinase phosphatase-1 (MKP-1) mRNA expression, which inhibits p-p38, was analyzed by means of real-time PCR. Glucocorticoid receptor (GR) binding and histone H4 acetylation in the glucocorticoid response element of the MKP-1 promoter in monocytes were analyzed by means of chromatin immunoprecipitation. Results DEX significantly inhibited LPS-induced p-p38 in monocytes from patients with SS asthma but not those from patients with SR asthma (P .01). VitD inhibited LPS-induced p-p38 in monocytes from both patient groups (P .01) but enhanced DEX suppression of LPS-induced p-p38 only in monocytes from patients with SS asthma (P .01). VitD induced MKP-1 expression and enhanced DEX induction of MKP-1 in both patients with SS asthma and patients with SR asthma. VitD/DEX-induced MKP-1 mRNA levels remained significantly lower in monocytes from patients with SR asthma (P .05). DEX-stimulated recruitment of GR and histone H4 acetylation at the glucocorticoid response element 4.6 kbp upstream of the MKP-1 gene were significantly lower in monocytes from patients with SR asthma compared with those from patients with SS asthma. VitD pretreatment enhanced DEX-induced GR binding and histone acetylation in monocytes from both patient groups. However, GR binding and histone H4 acetylation remained significantly lower in monocytes from patients with SR asthma. Conclusion VitD demonstrated anti-inflammatory and corticosteroid-enhancing effects in monocytes of patients with SR asthma and patients with SS asthma. However, the responses to corticosteroids in patients with SR asthma remained significantly lower than those in patients with SS asthma.
机译:背景技术维生素D以其抗炎作用而闻名。客观研究维生素D对类固醇抵抗性(SR)与类固醇敏感性(SS)哮喘患者反应的调节作用。方法对11例SR哮喘患者和8例SS哮喘患者的外周血细胞进行1,25-二羟基维生素D(1,25 [OH] 2D [VitD])的预培养,然后进行地塞米松(DEX)治疗和LPS刺激。通过流式细胞术检查LPS诱导的单核细胞中磷酸化的p38丝裂原活化蛋白激酶(p-p38)。通过实时PCR分析抑制p-p38的丝裂原活化蛋白激酶磷酸酶-1(MKP-1)mRNA表达。通过染色质免疫沉淀法分析了单核细胞中MKP-1启动子的糖皮质激素应答元件中糖皮质激素受体(GR)的结合和组蛋白H4乙酰化。结果DEX显着抑制了SS哮喘患者单核细胞中LPS诱导的p-p38,而不是SR哮喘患者单核细胞(P <.01)。 VitD抑制了两个患者组的单核细胞中LPS诱导的p-p38(P <.01),但仅增强了SS哮喘患者的单核细胞中LPS诱导的p-p38的DEX抑制(P <.01)。 VitD在SS哮喘患者和SR哮喘患者中均诱导了MKP-1表达并增强了MKP-1的DEX诱导。 SR哮喘患者的单核细胞中,VitD / DEX诱导的MKP-1 mRNA水平仍显着降低(P <.05)。与SS哮喘患者相比,SR哮喘患者的单核细胞中DEX刺激的GR和MKP-1基因上游4.6 kbp处糖皮质激素反应元件的组蛋白H4乙酰化显着降低。 VitD预处理增强了两个患者组的单核细胞中DEX诱导的GR结合和组蛋白乙酰化。但是,SR哮喘患者的单核细胞中GR结合和组蛋白H4乙酰化仍然显着降低。结论VitD对SR哮喘和SS哮喘患者的单核细胞具有抗炎和增强糖皮质激素的作用。然而,SR哮喘患者对皮质类固醇的反应仍然明显低于SS哮喘患者。

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