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首页> 美国卫生研究院文献>Journal of Virology >Cytokine-mediated induction of human immunodeficiency virus (HIV) expression and cell death in chronically infected U1 cells: do tumor necrosis factor alpha and gamma interferon selectively kill HIV-infected cells?
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Cytokine-mediated induction of human immunodeficiency virus (HIV) expression and cell death in chronically infected U1 cells: do tumor necrosis factor alpha and gamma interferon selectively kill HIV-infected cells?

机译:细胞因子介导的人类免疫缺陷病毒(HIV)的表达诱导和慢性感染的U1细胞中的细胞死亡:肿瘤坏死因子α和γ干扰素是否选择性杀死HIV感染的细胞?

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Infection with several DNA or RNA viruses induces a state of increased sensitivity to cell lysis mediated by tumor necrosis factor (TNF), particularly in the presence of gamma interferon (IFN-gamma). Infection of human cells with the human immunodeficiency virus (HIV) may induce a similar phenomenon. However, TNF and IFN-gamma are known upregulators of HIV replication, raising the question of the potential role of these cytokines in the selective elimination of cells infected with this virus. The present study demonstrates that chronically infected U1 cells were killed with much greater efficiency by costimulation with TNF-alpha and IFN-gamma than their uninfected parental cell line U937. However, synergistic induction of viral expression also occurred in U1 cells as a consequence of treatment with the two cytokines. Cell death in U1 cells was not caused by the massive production of virions, in that costimulation with glucocorticoid hormones and TNF-alpha or IFN-gamma resulted in high levels of virion production without cytopathicity. To investigate the nature of the selective cytotoxic effect observed in U1 cells costimulated with TNF-alpha plus IFN-gamma, a panel of uninfected cell clones was generated by limiting dilution of U937 cells and tested for response to TNF-alpha and/or IFN-gamma. In contrast to the uncloned bulk parental U937 cell line, most uninfected cell clones showed a very high susceptibility to being killed by TNF-alpha and IFN-gamma. Similar findings were obtained when both infected U1 cells and several uninfected U937 cell clones were costimulated with an anti-Fas monoclonal antibody in the presence of IFN-gamma, although, unlike cells stimulated with TNF-alpha, cells treated with anti-Fas antibody did not express virus. Therefore, the increased susceptibility to cytokine-mediated lysis observed in cell lines infected with HIV is likely due to the selection of preexisting cell clones rather than viral infection.
机译:感染数种DNA或RNA病毒后,会引起对由肿瘤坏死因子(TNF)介导的细胞裂解敏感性提高的状态,尤其是在存在γ干扰素(IFN-γ)的情况下。人类免疫缺陷病毒(HIV)感染人类细胞可能会诱发类似现象。然而,已知TNF和IFN-γ是HIV复制的上调剂,这提出了这些细胞因子在选择性清除被该病毒感染的细胞中的潜在作用的问题。本研究表明,与未感染的亲代细胞系U937相比,用TNF-α和IFN-γ共同刺激可以更有效地杀死慢性感染的U1细胞。然而,由于用两种细胞因子处理,在U1细胞中也发生了协同的病毒表达诱导。 U1细胞中的细胞死亡不是由病毒粒子的大量产生引起的,因为与糖皮质激素和TNF-α或IFN-γ的共刺激导致高水平的病毒粒子产生而没有细胞病变。为了研究在与TNF-α和IFN-γ共刺激的U1细胞中观察到的选择性细胞毒性作用的性质,通过限制稀释U937细胞来产生一组未感染的细胞克隆,并测试其对TNF-α和/或IFN-γ的反应伽玛与未克隆的大量亲本U937细胞系相反,大多数未感染的细胞克隆表现出极高的被TNF-α和IFN-γ杀死的敏感性。当存在IFN-γ的情况下同时使用抗Fas单克隆抗体共同感染U1细胞和几个未感染的U937细胞克隆时,也获得了类似的发现,尽管与用TNF-α刺激的细胞不同,用抗Fas抗体处理的细胞不表达病毒。因此,在HIV感染的细胞系中观察到的对细胞因子介导的裂解的敏感性增加可能是由于选择了已有的细胞克隆而不是病毒感染。

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