Haaland Ingvild, Opsahl Jill A, Berven Frode S, Reikvam Håkon, Fredly Hanne K, Haugse Ragnhild, Thiede Bernd, McCormack Emmet, Lain Sonia, Bruserud Oystein, Gjertsen Bjørn Tore
Department of Internal Medicine, Haukeland University Hospital, Bergen N-5021, Norway.
Mol Cancer. 2014 May 21;13:116. doi: 10.1186/1476-4598-13-116.
The small-molecule MDM2 antagonist nutlin-3 has proved to be an effective p53 activating therapeutic compound in several preclinical cancer models, including acute myeloid leukemia (AML). We and others have previously reported a vigorous acetylation of the p53 protein by nutlin-treatment. In this study we aimed to investigate the functional role of this p53 acetylation in nutlin-sensitivity, and further to explore if nutlin-induced protein acetylation in general could indicate novel targets for the enhancement of nutlin-based therapy.
Nutlin-3 was found to enhance the acetylation of p53 in the human AML cell line MOLM-13 (wild type TP53) and in TP53 null cells transfected with wild type p53 cDNA. Stable isotope labeling with amino acids in cell culture (SILAC) in combination with immunoprecipitation using an anti-acetyl-lysine antibody and mass spectrometry analysis identified increased levels of acetylated Histone H2B, Hsp27 and Hsp90 in MOLM-13 cells after nutlin-treatment, accompanied by downregulation of total levels of Hsp27 and Hsp90. Intracellular levels of heat shock proteins Hsp27, Hsp40, Hsp60, Hsp70 and Hsp90α were correlated to nutlin-sensitivity for primary AML cells (n = 40), and AML patient samples with low sensitivity to nutlin-3 tended to express higher levels of heat shock proteins than more responsive samples. Combination therapy of nutlin-3 and Hsp90 inhibitor geldanamycin demonstrated synergistic induction of apoptosis in AML cell lines and primary AML cells. Finally, TP53 null cells transfected with a p53 acetylation defective mutant demonstrated decreased heat shock protein acetylation and sensitivity to nutlin-3 compared to wild type p53 expressing cells.
Altogether, our results demonstrate that nutlin-3 induces acetylation of p53, histones and heat shock proteins, and indicate that p53 acetylation status and the levels of heat shock proteins may participate in modulation of nutlin-3 sensitivity in AML.
小分子MDM2拮抗剂Nutlin-3已被证明在包括急性髓系白血病(AML)在内的多种临床前癌症模型中是一种有效的p53激活治疗化合物。我们和其他人之前报道过,用Nutlin处理可使p53蛋白发生强烈乙酰化。在本研究中,我们旨在研究这种p53乙酰化在Nutlin敏感性中的功能作用,并进一步探讨Nutlin诱导的蛋白质乙酰化总体上是否可指示增强基于Nutlin治疗的新靶点。
发现Nutlin-3可增强人AML细胞系MOLM-13(野生型TP53)和转染了野生型p53 cDNA的TP53缺失细胞中p53的乙酰化。细胞培养中氨基酸的稳定同位素标记(SILAC)结合使用抗乙酰赖氨酸抗体的免疫沉淀和质谱分析,确定了用Nutlin处理后MOLM-13细胞中乙酰化组蛋白H2B、Hsp27和Hsp90水平升高,同时伴随着Hsp27和Hsp90总水平的下调。热休克蛋白Hsp27、Hsp40、Hsp60、Hsp70和Hsp90α的细胞内水平与原发性AML细胞(n = 40)对Nutlin的敏感性相关,对Nutlin-3敏感性低的AML患者样本往往比反应性更强的样本表达更高水平的热休克蛋白。Nutlin-3与Hsp90抑制剂格尔德霉素的联合治疗在AML细胞系和原发性AML细胞中显示出协同诱导凋亡的作用。最后,与表达野生型p53的细胞相比,转染了p53乙酰化缺陷突变体的TP53缺失细胞显示出热休克蛋白乙酰化减少和对Nutlin-3的敏感性降低。
总之,我们的结果表明Nutlin-3诱导p53、组蛋白和热休克蛋白的乙酰化,并表明p53乙酰化状态和热休克蛋白水平可能参与调节AML中对Nutlin-3的敏感性。
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