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Effects of systemic and neuraxial morphine on the immune system

机译:全身和神经吗啡对免疫系统的影响

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In the study, we tried to evaluate the effects of morphine injected through the systemic or neuraxial route on immune cell function and cytokine production in healthy women. In total, 29 paired samples of fresh peripheral blood were collected from healthy women who had been administered morphine for anesthetic analgesia through intravenous (IV), epidural, or spinal route postpartum. Their isolated peripheral blood mononuclear cells were mitogen-activated and stained with fluorochrome-conjugated anti-CD4, anti-CD8, anti-interleukin (IL)-2, and anti-interferon (IFN)-γ antibodies for flow cytometry, and the plasma levels of cytokines, including IL-6, IFN-α2, IL-10, IL-8, GM-CSF, and monocyte chemoattractant protein (MCP)-1, were measured through enzyme-linked immunosorbent assay. The results demonstrated that regardless of the administration route, morphine delivery slightly reduced IL-2 expression in CD4sup xmlns:mrws="http://webservices.ovid.com/mrws/1.0"+/sup cells after activation, and the same effect was not noted for CD8sup xmlns:mrws="http://webservices.ovid.com/mrws/1.0"+/sup cells. Intravenous or epidural morphine tended to reduce IFN-γ expression in CD8sup xmlns:mrws="http://webservices.ovid.com/mrws/1.0"+/sup cells. Spinal and IV morphine substantially increased IL-6 production, whereas epidural morphine hindered IL-10 and GM-CSF production. IV morphine injection reduced MCP-1 production in plasma. Compared with spinal morphine , IV or epidural morphine may more effectively inhibit the expression of various cytokines and thus affect immune response. All 3 routes of morphine injection tended to decrease IL-2 production by CD4sup xmlns:mrws="http://webservices.ovid.com/mrws/1.0"+/sup cells, whereas IV or epidural morphine injection showed lower IFN-γ production by CD8sup xmlns:mrws="http://webservices.ovid.com/mrws/1.0"+/sup cells. However, additional large-scale studies with longer follow-up durations are warranted.
机译:在这项研究中,我们试图评估通过全身或神经途径注射的吗啡对健康女性免疫细胞功能和细胞因子产生的影响。总共从健康妇女中收集了29对新鲜的外周血样本,这些妇女在产后通过静脉注射(IV),硬膜外或脊髓途径接受了吗啡镇痛。将其分离的外周血单核细胞进行促分裂原激活,并用荧光标记的抗CD4,抗CD8,抗白介素(IL)-2和抗干扰素(IFN)-γ抗体进行流式细胞仪染色,并进行血浆染色通过酶联免疫吸附测定法测定了包括IL-6,IFN-α2,IL-10,IL-8,GM-CSF和单核细胞趋化蛋白(MCP)-1在内的细胞因子的水平。结果表明,无论给药途径如何,激活后吗啡传递都会使CD4 + 细胞中的IL-2表达略有降低。 ,而对于CD8 + 单元,则没有注意到相同的效果。静脉或硬膜外吗啡倾向于减少CD8 + 细胞中的IFN-γ表达。脊髓和静脉注射吗啡会显着增加IL-6的产生,而硬膜外吗啡会阻碍IL-10和GM-CSF的产生。静脉注射吗啡可减少血浆中MCP-1的产生。与脊髓吗啡相比,静脉或硬膜外吗啡可以更有效地抑制各种细胞因子的表达,从而影响免疫反应。吗啡注射的所有3种途径均倾向于通过CD4 + 细胞降低IL-2的产生,而静脉注射或硬膜外注射吗啡结果显示CD8 + 细胞产生的IFN-γ降低。但是,需要进行更多的随访时间较长的大规模研究。

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