首页> 外文期刊>Biochimica et biophysica acta. Molecular cell research >Oncogenic acidic nuclear phosphoproteins ANP32C/D are novel clients of heat shock protein 90
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Oncogenic acidic nuclear phosphoproteins ANP32C/D are novel clients of heat shock protein 90

机译:致癌性酸性核磷蛋白ANP32C / D是热激蛋白90的新客户

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摘要

The acidic nuclear phosphoproteins (ANP32A-H) are an evolutionarily conserved family of proteins with diverse and sometimes opposing cellular functions. Here we show that the oncogenic family members ANP32C and ANP32D are associated in complexes containing the molecular chaperone Hsp90. The oncogenic ANP32C protein appears to be highly unstable with a rapid degradation (t(1/2) > 30 min) occurring upon treatment of cells with cycloheximide. ANP32C was also found to be associated with oncogenic Hsp90 complexes by virtue of its ability to interact and be immunoprecipitated by the Hsp90 inhibitor PU-H71. Further studies treating cells with the Hsp90 inhibitors PU-H71 and 17-AAG showed atypical increased protein stability and prevention of ANP32C degradation compared to the Hsp90 client AKT. Cells overexpressing ANP32C or its mutant ANP32CY140H showed enhanced sensitivity to treatment with PU-H71 as demonstrated by CCK-8 and colony formation assays. Our results highlight that certain malignancies with ANP32C/D overexpression or mutation might be specifically targeted using Hsp90 inhibitors. (C) 2015 Elsevier B.V. All rights reserved.
机译:酸性核磷蛋白(ANP32A-H)是进化上保守的蛋白质家族,具有多种多样且有时相反的细胞功能。在这里,我们显示致癌家族成员ANP32C和ANP32D在包含分子伴侣Hsp90的复合物中相关。用环己酰亚胺处理细胞后,致癌的ANP32C蛋白似乎高度不稳定,并发生快速降解(t(1/2)> 30分钟)。还发现ANP32C由于其与Hsp90抑制剂PU-H71相互作用并被其免疫沉淀的能力,与致癌的Hsp90复合物有关。与Hsp90客户AKT相比,用Hsp90抑制剂PU-H71和17-AAG处理细胞的进一步研究表明,蛋白质稳定性非典型地增加,并防止了ANP32C降解。如CCK-8和集落形成试验所示,过表达ANP32C或其突变体ANP32CY140H的细胞显示出对PU-H71处理的敏感性增强。我们的结果表明,使用Hsp90抑制剂可特异性靶向某些具有ANP32C / D过表达或突变的恶性肿瘤。 (C)2015 Elsevier B.V.保留所有权利。

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