Murphy Amanda J, Hughes Caroline A, Barrett Ciara, Magee Hilary, Loftus Barbara, O'Leary John J, Sheils Orla
Department of Cellular Pathology, Adelaide and Meath Hospital, Trinity College, Dublin, Ireland.
Cancer Res. 2007 Mar 15;67(6):2893-8. doi: 10.1158/0008-5472.CAN-06-2962.
HER2 and TOP2A genes, located on 17q, can be coamplified in cancer. Overexpression of both genes has been reported in high-grade, androgen-resistant prostate cancer. Both genes have not been compared in a single prostate cancer study and the frequency of TOP2A amplifications in prostate cancer is unknown. Using tissue microarrays, we did immunohistochemistry and fluorescence in situ hybridization for HER2 and TOP2A in 100 prostate cancers (41 localized and 59 advanced) and 42 cases of benign prostatic hyperplasia (BPH). Amplification was defined as a target/centromere signal ratio of > or =1.5. HER2 immunohistochemistry was scored from 0 to 3+. Percentage nuclei staining for topoisomerase IIalpha (topoIIalpha) was recorded; overexpression was defined as > or =5% cells staining. Eighteen (31%) advanced prostate cancers showed topoIIalpha overexpression; 12 (26%) showed TOP2A low-level amplification; 9 (16%) expressed HER2; and 6 (13%) showed HER2 low-level amplification. No high-level amplification of either gene (target/centromere signal ratio of > or =3.0) was detected. TOP2A coexpression and coamplification were seen in 75% and 66% of HER2-positive cases, respectively. Localized prostate cancer or BPH showed no gene amplification or topoIIalpha overexpression. Gene amplification or overexpression correlated with high stage and Gleason score. The presence of TOP2A amplification in advanced cancer was associated with androgen resistance and decreased survival by multivariate analysis. This is the first study to document low-level TOP2A amplification in prostate cancer and an association with reduced survival. TOP2A amplification may occur with or without HER2 duplication and is often associated with topoIIalpha expression. Therapies directed against topoIIalpha (and HER2) in such patients may improve survival.
位于17号染色体长臂(17q)上的HER2和TOP2A基因在癌症中可能会共同扩增。在高级别、雄激素抵抗性前列腺癌中,已报道这两种基因均过表达。在单一的前列腺癌研究中,尚未对这两种基因进行比较,且前列腺癌中TOP2A扩增的频率尚不清楚。我们使用组织微阵列,对100例前列腺癌(41例局限性癌和59例进展期癌)以及42例良性前列腺增生(BPH)病例进行了HER2和TOP2A的免疫组织化学及荧光原位杂交检测。扩增被定义为靶标/着丝粒信号比≥1.5。HER2免疫组织化学评分从0到3+。记录拓扑异构酶IIα(topoIIα)的细胞核染色百分比;过表达被定义为≥5%的细胞染色。18例(31%)进展期前列腺癌显示topoIIα过表达;12例(26%)显示TOP2A低水平扩增;9例(16%)表达HER2;6例(13%)显示HER2低水平扩增。未检测到任何一种基因的高水平扩增(靶标/着丝粒信号比≥3.0)。在HER2阳性病例中,分别有75%和66%观察到TOP2A共表达和共扩增。局限性前列腺癌或BPH未显示基因扩增或topoIIα过表达。基因扩增或过表达与高分期和 Gleason评分相关。多因素分析显示,进展期癌症中TOP2A扩增的存在与雄激素抵抗及生存率降低相关。这是第一项记录前列腺癌中TOP2A低水平扩增及其与生存率降低相关的研究。TOP2A扩增可能在有或无HER2复制的情况下发生,且常与topoIIα表达相关。针对此类患者的topoIIα(和HER2)靶向治疗可能会改善生存率。
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