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首页> 外文期刊>Gene: An International Journal Focusing on Gene Cloning and Gene Structure and Function >Regulation of interlocking gene regulatory network subcircuits by a small molecule inhibitor of retinoblastoma protein (RB) phosphorylation: Cancer cell expression of HLA-DR
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Regulation of interlocking gene regulatory network subcircuits by a small molecule inhibitor of retinoblastoma protein (RB) phosphorylation: Cancer cell expression of HLA-DR

机译:视网膜母细胞瘤蛋白(RB)磷酸化的小分子抑制剂对连锁基因调控网络子回路的调控:HLA-DR的癌细胞表达

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摘要

The induction of the major histocompatibility (MHC), antigen-presenting class II molecules by interferon-gamma, in solid tumor cells, requires the retinoblastoma tumor suppressor protein (Rb). In the absence of Rb, a repressosome blocks the access of positive-acting, promoter binding proteins to the MHC class II promoter. However, a complete molecular linkage between Rb expression and the disassembly of the MHC class II repressosome has been lacking. By treating A549 lung carcinoma cells with a novel small molecule that prevents phosphorylation-mediated, Rb inactivation, we demonstrate that Rb represses the synthesis of an MHC class II repressosome component, YY1. The reduction in YY1 synthesis correlates with the advent of MHC class II inducibility; with loss of YY1 binding to the promoter of the HLA-DRA gene, the canonical human MHC class II gene; and with increased Rb binding to the YY1 promoter. These results support the concept that the Rb gene regulatory network (GRN) subcircuit that regulates cell proliferation is linked to a GRN subcircuit regulating a tumor cell immune function.
机译:干扰素-γ在实体瘤细胞中诱导主要组织相容性(MHC),即抗原呈递II类分子,需要视网膜母细胞瘤抑癌蛋白(Rb)。在没有Rb的情况下,阻遏物会阻止正向启动子结合蛋白与MHC II类启动子的接触。但是,Rb表达和MHC II类repressosome的拆卸之间缺乏完整的分子联系。通过用防止磷酸化介导的Rb失活的新型小分子治疗A549肺癌细胞,我们证明Rb抑制II类MHC抑制因子YY1的合成。 YY1合成的减少与II类MHC诱导能力的出现有关。 YY1与HLA-DRA基因(人类典型MHC II类基因)启动子的结合丧失;并且Rb与YY1启动子的结合增加。这些结果支持这样的概念,即调节细胞增殖的Rb基因调节网络(GRN)子电路与调节肿瘤细胞免疫功能的GRN子电路相连。

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