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PPM1D gene amplification and overexpression in breast cancer: a qRT-PCR and chromogenic in situ hybridization study

机译:乳腺癌中PPM1D基因的扩增和过表达:qRT-PCR和生色原位杂交研究

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PPM1D (protein phosphatase magnesium-dependent 1δ) maps to the 17q23.2 amplicon and is amplified in ~8% of breast cancers. The PPM1D gene encodes a serine threonine phosphatase, which is involved in the regulation of several tumour suppressor pathways, including the p53 pathway. Along with others, we have recently shown that PPM1D is one of the drivers of the 17q23.2 amplicon and a promising therapeutic target. Here we investigate whether PPM1D is overexpressed when amplified in breast cancers and the correlations between PPM1D overexpression and amplification with clinicopathological features and survival of breast cancer patients from a cohort of 245 patients with invasive breast cancer treated with therapeutic surgery followed by adjuvant anthracycline-based chemotherapy. mRNA was extracted from representative sections of tumours containing >50% of tumour cells and subjected to TaqMan quantitative real-time PCR using primers for PPM1D and for two housekeeping genes. PPM1D overexpression was defined as the top quartile of expression levels. Chromogenic in situ hybridization with in-house-generated probes for PPM1D was performed. Amplification was defined as >50% of cancer cells with >5 signals per nucleus/large gene clusters. PPM1D overexpression and amplification were found in 25 and 6% of breast cancers, respectively. All cases harbouring PPM1D amplification displayed PPM1D overexpression. PPM1D overexpression was inversely correlated with expression of TOP2A, EGFR and cytokeratins 5/6 and 17. PPM1D amplification was significantly associated with HER2 overexpression, and HER2, TOP2A and CCND1 amplification. No association between PPM1D gene amplification and PPM1D mRNA overexpression with survival was observed. In conclusion, PPM1D is consistently overexpressed when amplified; however, PPM1D overexpression is more pervasive than gene amplification. PPM1D overexpression and amplification are associated with tumours displaying luminal or HER2 phenotypes. Co-amplification of PPM1D and HER2/TOP2A and CCND1 are not random events and may suggest the presence of a ‘firestorm’ genetic profile.
机译:PPM1D(蛋白质磷酸酶镁依赖性1δ)定位于17q23.2扩增子,在约8%的乳腺癌中被扩增。 PPM1D基因编码丝氨酸苏氨酸磷酸酶,其参与多种肿瘤抑制途径的调控,包括p53途径。与其他人一起,我们最近发现PPM1D是17q23.2扩增子的驱动程序之一,也是有希望的治疗靶标。在这里,我们研究了245例浸润性乳腺癌患者中,经治疗性手术后辅以蒽环类辅助化疗的人群,是否在乳腺癌中扩增时PPM1D是否过表达,以及PPM1D过表达和扩增与乳腺癌的临床病理特征和生存之间的相关性。从包含> 50%肿瘤细胞的肿瘤代表性切片中提取mRNA,并使用PPM1D和两个看家基因的引物进行TaqMan定量实时PCR。 PPM1D过表达定义为表达水平的最高四分位数。使用内部生成的PPM1D探针进行显色原位杂交。扩增定义为癌细胞的> 50%,每个细胞核/大基因簇的信号> 5。 PPM1D过表达和扩增分别在25%和6%的乳腺癌中发现。所有携带PPM1D扩增的病例均显示PPM1D过表达。 PPM1D过表达与TOP2A,EGFR和细胞角蛋白5/6和17的表达呈负相关。PPM1D扩增与HER2过表达,HER2,TOP2A和CCND1扩增显着相关。没有观察到PPM1D基因扩增和PPM1D mRNA过表达与生存之间的关联。总之,PPM1D在扩增时始终过表达。但是,PPM1D过表达比基因扩增更普遍。 PPM1D过表达和扩增与显示腔或HER2表型的肿瘤有关。 PPM1D和HER2 / TOP2A和CCND1的共同扩增不是随机事件,可能表明存在“风暴”遗传图谱。

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