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使用芳香化酶抑制剂来曲唑治疗后乳腺癌转录谱的变化。

Changes in breast cancer transcriptional profiles after treatment with the aromatase inhibitor, letrozole.

作者信息

Miller William R, Larionov Alexey A, Renshaw Lorna, Anderson Thomas J, White Sharon, Murray Juliette, Murray Emma, Hampton Garret, Walker John R, Ho Steven, Krause Andreas, Evans Dean B, Dixon John Michael

机构信息

Breast Research Group, University of Edinburgh, Edinburgh, UK.

出版信息

Pharmacogenet Genomics. 2007 Oct;17(10):813-26. doi: 10.1097/FPC.0b013e32820b853a.

Abstract

OBJECTIVE

The aim of the study was to identify changes in tumour expression profiling associated with short-term therapy of breast cancer patients with letrozole.

EXPERIMENTAL DESIGN

Microarray analysis was performed on RNA extracted from paired tumour core biopsies taken before and after 14 days of treatment with letrozole (2.5 mg/daily) in 58 patients. Changes in expression profile were identified by three different approaches on the basis of frequency of changes, magnitude of changes and significance analysis of microarray.

RESULTS

No single gene was consistently changed by therapy in all cases. Fifty-two genes, however, were downregulated and 36 upregulated in at least 45 of the 58 cases. In terms of quantitative change, 46 genes showed at least a median 1.5-fold change in expression. Significance analysis of microarray identified 62 genes that were significantly changed by therapy (P<0.0001, 56 downregulated and six upregulated). All three approaches showed that greater numbers of genes were downregulated rather than upregulated. Merging data produced a total of 143 genes, which were subject to gene ontology and cluster analysis. The ontology of the 91 downregulated genes showed that they were functionally associated with cell cycle progression, particularly mitosis. In contrast, upregulated genes were associated with organ development, connective tissue extracellular matrix regulation and inflammatory response. Cluster analysis segregated the patients into four groups differing in patterns of gene expression.

CONCLUSION

Genes have been identified which either change markedly or consistently in breast cancer after 14 days treatment with letrozole. These are new important data in understanding letrozole's molecular mechanism of action in breast cancers.

摘要

目的

本研究旨在确定来曲唑短期治疗乳腺癌患者后肿瘤表达谱的变化。

实验设计

对58例患者在接受来曲唑(2.5mg/日)治疗14天前后采集的配对肿瘤芯针活检组织中提取的RNA进行微阵列分析。基于变化频率、变化幅度和微阵列的显著性分析,通过三种不同方法确定表达谱的变化。

结果

在所有病例中,没有单个基因因治疗而持续发生变化。然而,在58例中的至少45例中,有52个基因下调,36个基因上调。就定量变化而言,46个基因的表达至少有中位数1.5倍的变化。微阵列显著性分析确定了62个因治疗而显著变化的基因(P<0.0001,56个下调,6个上调)。所有三种方法均显示下调的基因数量多于上调的基因。合并数据共产生143个基因,对其进行基因本体论和聚类分析。91个下调基因的本体论显示它们在功能上与细胞周期进程相关,尤其是有丝分裂。相比之下,上调基因与器官发育、结缔组织细胞外基质调节和炎症反应相关。聚类分析将患者分为四组,基因表达模式不同。

结论

已确定在接受来曲唑治疗14天后乳腺癌中显著或持续变化的基因。这些是理解来曲唑在乳腺癌中分子作用机制的重要新数据。

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