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首页> 外文期刊>Clinical immunology: The official journal of the Clinical Immunology Society >Involvement of the TNF-alpha autocrine-paracrine loop, via NF-kappaB and YY1, in the regulation of tumor cell resistance to Fas-induced apoptosis.
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Involvement of the TNF-alpha autocrine-paracrine loop, via NF-kappaB and YY1, in the regulation of tumor cell resistance to Fas-induced apoptosis.

机译:TNF-α自分泌-旁分泌环通过NF-κB和YY1参与调节肿瘤细胞对Fas诱导的细胞凋亡的抗性。

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Many tumors are resistant to Fas ligand (FasL)-induced apoptosis. This study examined the role of tumor-derived TNF-alpha, via an autocrine/paracrine loop, in the regulation of tumor-cell resistance to FasL-induced apoptosis. We have reported that Fas expression and sensitivity to FasL is negatively regulated by the transcription repressor factor Yin Yang 1 (YY1). Thus, we hypothesized that tumor-derived TNF-alpha induces the activation of NF-kappaB and the transcription repressor YY1, both of which negatively regulate Fas expression and sensitivity to FasL-induced apoptosis. This hypothesis was tested in PC-3 prostate cancer cells which synthesize and secrete TNF-alpha and express constitutively active NF-kappaB and YY1. Treatment of PC-3 cells with TNF-alpha (10 units) resulted in increased NF-kappaB and YY1 DNA-binding activity, upregulation of YY1 expression, downregulation of surface and total Fas expression and enhanced resistance of PC-3 to apoptosis induced by the FasL agonist antibody CH-11. In contrast, blocking the binding of secreted TNF-alpha on PC-3 cells with soluble recombinant sTNF-RI resulted in significant inhibition of constitutive NF-kappaB and YY1 DNA-binding activity, downregulation of YY1 expression, upregulation of Fas expression and sensitization of tumor cells to CH-11-induced apoptosis. The regulation of YY1 expression and activity by NF-kappaB was demonstrated by the use of the NF-kappaB inhibitor Bay 11-7085 and by the use of a GFP reporter system whereby deletion of the YY1-tandem binding site in the promoter significantly enhanced GFP expression. The direct role of YY1 expression in the regulation of PC-3 resistance to CH-11-induced apoptosis was shown in cells transfected with siRNA YY1 whereby such cells exhibited upregulation of Fas expression and were sensitized to CH-11-induced apoptosis. These findings demonstrate that the TNF-alpha autocrine-paracrine loop is involved in the constitutive activation of the transcription factors NF-kappaB and YY1 in the tumor cells andthis loop leads to inhibition of Fas expression and resistance to FasL-induced apoptosis. Further, these findings identify new targets such as TNF-alpha, NF-kappaB and YY1, whose inhibition can reverse tumor cell resistance to FasL-mediated apoptosis.
机译:许多肿瘤对Fas配体(FasL)诱导的细胞凋亡具有抗性。这项研究通过自分泌/旁分泌环研究了肿瘤来源的TNF-α在调节肿瘤细胞对FasL诱导的细胞凋亡的抗性中的作用。我们已经报道,转录抑制因子Yin Yang 1(YY1)负调控Fas表达和对FasL的敏感性。因此,我们假设肿瘤来源的TNF-α诱导NF-κB和转录阻遏物YY1的激活,二者均负调控Fas表达和对FasL诱导的细胞凋亡的敏感性。在PC-3前列腺癌细胞中测试了该假设,该PC-3前列腺癌细胞合成并分泌TNF-α,并表达组成型活性NF-kappaB和YY1。用TNF-α(10个单位)处理PC-3细胞可导致NF-kappaB和YY1 DNA结合活性增加,YY1表达上调,表面和总Fas表达下调以及PC-3对由ATP诱导的凋亡的抵抗力增强FasL激动剂抗体CH-11。相反,用可溶性重组sTNF-RI阻断PC-3细胞上分泌的TNF-α的结合会显着抑制组成型NF-kappaB和YY1 DNA的结合活性,下调YY1表达,上调Fas表达和敏化肿瘤细胞以CH-11-诱导凋亡。通过使用NF-kappaB抑制剂Bay 11-7085和使用GFP报告系统证明了NF-kappaB对YY1表达和活性的调节,由此启动子中YY1串联结合位点的缺失显着增强了GFP表达。在用siRNA YY1转染的细胞中显示了YY1表达在调节PC-3对CH-11-诱导的凋亡的抗性中的直接作用,由此此类细胞表现出Fas表达的上调并且对CH-11-诱导的凋亡敏感。这些发现表明,TNF-α自分泌-旁分泌环参与肿瘤细胞中转录因子NF-κB和YY1的组成性活化,并且该环导致Fas表达的抑制和对FasL诱导的细胞凋亡的抵抗。此外,这些发现确定了新的靶标,例如TNF-α,NF-κB和YY1,它们的抑制作用可以逆转肿瘤细胞对FasL介导的细胞凋亡的抵抗力。

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