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首页> 美国卫生研究院文献>other >Dynorphin 1-17 and Its N-Terminal Biotransformation Fragments Modulate Lipopolysaccharide-Stimulated Nuclear Factor-kappa B Nuclear Translocation Interleukin-1beta and Tumor Necrosis Factor-alpha in Differentiated THP-1 Cells
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Dynorphin 1-17 and Its N-Terminal Biotransformation Fragments Modulate Lipopolysaccharide-Stimulated Nuclear Factor-kappa B Nuclear Translocation Interleukin-1beta and Tumor Necrosis Factor-alpha in Differentiated THP-1 Cells

机译:强啡肽1-17及其N末端生物转化片段调节脂多糖刺激的核因子κB核易位白介素1beta和肿瘤坏死因子-α在分化的THP-1细胞中。

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Dynorphin 1–17, (DYN 1–17) opioid peptide produces antinociception following binding to the kappa-opioid peptide (KOP) receptor. Upon synthesis and release in inflamed tissues by immune cells, DYN 1–17 undergoes rapid biotransformation and yields a unique set of opioid and non-opioid fragments. Some of these major fragments possess a role in immunomodulation, suggesting that opioid-targeted therapeutics may be effective in diminishing the severity of inflammatory disorders. This study aimed to examine the immunomodulatory effects of DYN 1–17 and major N-terminal fragments found in the inflammatory environment on nuclear factor-kappaB/p65 (NF-κB/p65) nuclear translocation and the release of interleukin-1beta (IL-1β) and tumor necrosis factor-alpha (TNF-α) from lipopolysaccharide (LPS)-stimulated, differentiated THP-1 cells. The results demonstrate that NF-κB/p65 nuclear translocation was significantly attenuated following treatment with DYN 1–17 and a specific range of fragments, with the greatest reduction observed with DYN 1–7 at a low concentration (10 nM). Antagonism with a selective KOP receptor antagonist, ML-190, significantly reversed the inhibitory effects of DYN 1–17, DYN 1–6, DYN 1–7 and DYN 1–9, but not other DYN 1–17 N-terminal fragments (DYN 1–10 and 1–11) on NF-κB/p65 nuclear translocation. DYN 1–17 and selected fragments demonstrated differential modulation on the release of IL-1β and TNF-α with significant inhibition observed with DYN 1–7 at low concentrations (1 nM and 10 pM). These effects were blocked by ML-190, suggesting a KOP receptor-mediated pathway. The results demonstrate that DYN 1–17 and certain N-terminal fragments, produced in an inflamed environment, play an anti-inflammatory role by inhibiting NF-κB/p65 translocation and the subsequent cytokine release through KOP receptor-dependent and independent pathways.
机译:强啡肽1–17(DYN 1–17)阿片肽在与κ阿片肽(KOP)受体结合后产生抗伤害作用。通过免疫细胞在发炎组织中合成和释放后,DYN 1-17会经历快速的生物转化,并产生一组独特的阿片样物质和非阿片样物质片段。这些主要片段中的一些在免疫调节中起作用,这表明以阿片样物质为靶点的治疗剂可能有效地减轻了炎症性疾病的严重性。这项研究旨在研究DYN 1-17和在炎症环境中发现的主要N末端片段对核因子-κB/ p65(NF-κB/ p65)核转运和白介素-1β(IL- 1β)和肿瘤坏死因子-α(TNF-α)来自脂多糖(LPS)刺激的,分化的THP-1细胞。结果表明,用DYN 1–17和特定范围的片段处理后,NF-κB/ p65的核转运显着减弱,在低浓度(10 nM)下用DYN 1–7观察到最大的减少。与选择性KOP受体拮抗剂ML-190的拮抗作用可显着逆转DYN 1–17,DYN 1–6,DYN 1–7和DYN 1–9的抑制作用,但不会破坏其他DYN 1–17 N末端片段( DYN 1-10和1-11)对NF-κB/ p65核易位。 DYN 1–17和选定的片段显示出对IL-1β和TNF-α释放的差异调节,在低浓度(1 nM和10 pM)下使用DYN 1–7观察到明显的抑制作用。这些作用被ML-190阻断,表明KOP受体介导的途径。结果表明,在发炎的环境中产生的DYN 1-17和某些N末端片段通过抑制NF-κB/ p65易位以及随后通过KOP受体依赖性和独立途径释放的细胞因子发挥抗炎作用。

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