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首页> 美国卫生研究院文献>PLoS Clinical Trials >Concurrent Treatment with Taxifolin and Cilostazol on the Lowering of β-Amyloid Accumulation and Neurotoxicity via the Suppression of P-JAK2/P-STAT3/NF-κB/BACE1 Signaling Pathways
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Concurrent Treatment with Taxifolin and Cilostazol on the Lowering of β-Amyloid Accumulation and Neurotoxicity via the Suppression of P-JAK2/P-STAT3/NF-κB/BACE1 Signaling Pathways

机译:紫杉醇和西洛他唑同时治疗通过抑制P-JAK2 / P-STAT3 /NF-κB/ BACE1信号通路降低β-淀粉样蛋白积累和神经毒性

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Taxifolin is a potent flavonoid that exerts anti-oxidative effect, and cilostazol increases intracellular cAMP levels by inhibiting phosphodiesterase 3 that shows antiinflammatory actions. BACE1 (β-site APP cleaving enzyme 1) is the rate-limiting enzyme responsible for the β-cleavage of amyloid precursor proteins to Aβ peptides. In this study, endogenous Aβ and C99 accumulation was explored in N2a Swe cells exposed to 1% FBS medium. Increased Aβ and C99 levels were significantly attenuated by taxifolin alone and in combination with cilostazol. Increased phosphorylated JAK2 at Tyr1007/1008 (P-JAK), phosphorylated STAT3 at Tyr 705 (P-STAT3) expressions and increased expressions of BACE1 mRNA and protein in the activated N2a Swe cells were significantly attenuated by taxifolin (10~50 μM), cilostazol (10~50 μM) alone and in combination at minimum concentrations. In these cells, decreased cytosol IκBα expression was elevated, and increased nuclear NF-κB p65 level and nuclear NF-κB p65 DNA binding activity were significantly reduced by taxifolin and cilostazol in a similar manner. Following STAT3 gene (~70% reduction) knockdown in N2a cells, Aβ-induced nuclear NF-κB and BACE1 expressions were not observed. Taxifolin, cilostazol, or resveratrol significantly stimulated SIRT1 protein expression. In SIRT1 gene-silenced (~50%) N2a cells, taxifolin, cilostazol, and resveratrol all failed to suppress Aβ1-42-stimulated P-STAT3 and BACE1 expression. Consequently, taxifolin and cilostazol were found to significantly decrease lipopolysaccharide (1–10 μg/ml)-induced iNOS and COX-2 expressions, and nitrite production in cultured BV-2 microglia cells and to increase N2a cell viability. In conclusion, taxifolin and cilostazol strongly inhibited amyloidogenesis in a synergistic manner by suppressing P-JAK2/P-STAT3-coupled NF-κB-linked BACE1 expression via the up-regulation of SIRT1.
机译:Taxifolin是一种有效的类黄酮,具有抗氧化作用,西洛他唑可通过抑制磷酸二酯酶3(显示抗炎作用)来提高细胞内cAMP水平。 BACE1(β位APP裂解酶1)是限速酶,负责将淀粉样前体蛋白β裂解为Aβ肽。在这项研究中,在暴露于1%FBS培养基的N2a Swe细胞中探索了内源性Aβ和C99积累。单独和联合西洛他唑的滑石粉可显着减弱Aβ和C99水平的升高。激活的N2a Swe细胞中Tyr1007 / 1008的磷酸化JAK2升高(P-JAK),Tyr 705的磷酸化STAT3(P-STAT3)表达以及BACE1 mRNA和蛋白的表达被滑石粉显着减弱(10〜50μM),西洛他唑(10〜50μM)单独使用或以最低浓度组合使用。在这些细胞中,滑石粉和西洛他唑以类似的方式显着降低了降低的细胞溶质IκBα表达,并显着降低了核NF-κBp65水平和核NF-κBp65 DNA结合活性。在N2a细胞中激活STAT3基因(减少约70%)后,未观察到Aβ诱导的核NF-κB和BACE1表达。紫杉醇,西洛他唑或白藜芦醇可显着刺激SIRT1蛋白表达。在沉默了SIRT1基因的N2a细胞(〜50%)中,滑石粉,西洛他唑和白藜芦醇均不能抑制Aβ1-42刺激的P-STAT3和BACE1的表达。因此,发现滑石粉和西洛他唑可显着降低脂多糖(1-10μg/ ml)诱导的iNOS和COX-2表达,并在培养的BV-2小胶质细胞中产生亚硝酸盐并增加N2a细胞活力。总之,滑石粉和西洛他唑通过上调SIRT1抑制P-JAK2 / P-STAT3偶联的NF-κB连接的BACE1表达,从而以协同方式强烈抑制淀粉样蛋白生成。

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