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Cytosolic‐nuclear Tumor Promoter‐specific Binding Protein: Association with the 90 kDa Heat Shock Protein and Translocation into Nuclei by Treatment with 12‐O‐Tetradecanoylphorbol 13‐Acetate

机译:胞核肿瘤肿瘤启动子特异性结合蛋白:与90 kDa热休克蛋白缔合并通过12-O-四氢十八碳酰佛波醇13-乙酸盐处理而转移到核中

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摘要

Suspension‐cultured HeLa cells possess a cytosolic‐nuclear tumor promoter‐specific binding protein (CN‐TPBP) which lacks protein kinase C activity. This CN‐TPBP existed in cytosol of HeLa cells, but translocated into nuclear fraction of the cells after treatment of the cells with 12‐O‐tetradecanoyl‐phorbol 13‐acetate (TPA). The translation of CN‐TPBP induced by TPA became apparent within 10 min after the treatment with TPA, and was completed within 3 h. CN‐TPBP bound TPA with the association constant of 1.4X1010M−1, and also bound teleocidin B, debromoaplysiatoxin, and thapsigargin in a mutually competitive manner. The binding affinity order of synthetic analogs of teleocidin B correlated with the adhesion‐inducing potency order of the compounds toward human leukemia cell line HL‐60. The apparent molecular weight of CN‐TPBP under non‐denaturing conditions was estimated to be 66–68 kDa. CN‐TPBP forms a complex with the 90 kDa heat shock protein, and the complex was stabilized by the presence of molybdate. These characteristics of CN‐TPBP are similar to those of the nuclear receptors of glucocorticoid and dioxin. These findings suggested that CN‐TPBP acts as a nuclear receptor for tumor promoters, and that tumor promoters may exert their biological effects by binding to CN‐TPBP.
机译:悬浮培养的HeLa细胞具有胞质核肿瘤启动子特异性结合蛋白(CN-TPBP),该蛋白缺乏蛋白激酶C活性。该CN‐TPBP存在于HeLa细胞的细胞溶质中,但在用12‐O‐十四烷酰‐佛波醇13‐醋酸盐(TPA)处理细胞后易位到细胞的核部分中。由TPA诱导的CN‐TPBP的翻译在TPA处理后的10分钟内变得明显,并在3小时内完成。 CN‐TPBP以1.4X10 10 M -1 的缔合常数结合TPA,并以相互竞争的方式结合电离蛋白B,去溴卵磷脂和毒胡萝卜素。 teleoocidin B合成类似物的结合亲和力顺序与化合物对人白血病细胞系HL-60的黏附诱导能力顺序有关。在非变性条件下,CN-TPBP的表观分子量估计为66-68 kDa。 CN‐TPBP与90 kDa热激蛋白形成复合物,并且该复合物因存在钼酸盐而稳定。 CN‐TPBP的这些特征与糖皮质激素和二恶英的核受体相似。这些发现表明,CN‐TPBP充当肿瘤启动子的核受体,并且肿瘤启动子可能通过与CN‐TPBP结合而发挥其生物学作用。

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