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首页> 外文期刊>Breast Cancer Research and Treatment >Gene expression profiling and prediction of response to hormonal neoadjuvant treatment with anastrozole in surgically resectable breast cancer
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Gene expression profiling and prediction of response to hormonal neoadjuvant treatment with anastrozole in surgically resectable breast cancer

机译:可手术切除的乳腺癌的基因表达谱分析和阿那曲唑对激素新辅助治疗的反应预测

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Aromatase inhibition (AI) is the most effective endocrine treatment for breast cancer in post-menopausal patients, but a percentage of hormone receptor-positive cancers do not benefit from such therapy: for example, about 20% of patients treated with anastrozole do not respond and it is still impossible to accurately predict sensitivity. Our main goal was to identify a robust expression signature predictive of response to neoadjuvant treatment with anastrozole in patients with ER+ breast cancer. At the same time, we addressed the question of delineating treatment effects and possible mechanisms of intrinsic resistance occurring in non-responder patients. We analyzed the transcriptome of 17 tru-cut biopsies before treatment and 13 matched surgical samples after 3 months treatment with anastrozole taken from ER+ breast tumors. Molecular profiles were related to clinical response data. Treatment with anastrozole was associated with a decreased expression of genes relating to cell proliferation and an increased expression of genes relating to inflammatory processes. There was also an enrichment of induction of T-cell anergy, positive regulation of androgen signalling, synaptic transmission and vesicle trafficking in non-responders, and of cell cycle inhibition and induction of immune response in responders. We identified an expression signature of 77 probes (54 genes) that predicted response in 100% of our cases. Five of them were able to accurately predict response on an independent dataset (P = 0.0056) of 52 ER+ breast cancers treated with letrozole. Ten fixed independent samples from the anastrozole study were also used for RT-qPCR validations. This study suggests that a relative small number of genes analysed in a pre-treatment biopsy may identify patients likely to respond to AI neoadjuvant treatment. This may have practical utility translatable to the clinics. Furthermore, it delineates novel mechanisms of intrinsic resistance to AI therapy that could be further investigated in order to explore circumventing treatments.
机译:芳香酶抑制(AI)是绝经后乳腺癌中最有效的内分泌治疗方法,但一定比例的激素受体阳性癌症不能从这种治疗中受益:例如,约20%接受阿那曲唑治疗的患者对此无反应而且仍然无法准确预测灵敏度。我们的主要目标是鉴定出能预测ER +乳腺癌患者对阿那曲唑新辅助治疗反应的稳健表达特征。同时,我们解决了划定治疗效果以及无反应患者发生内在耐药的可能机制的问题。我们分析了治疗前17份tru-cut活检的转录组,以及3个月后用取自ER +乳腺肿瘤的阿那曲唑治疗后的13份匹配的手术样品的转录组。分子谱与临床反应数据有关。用阿那曲唑治疗与细胞增殖相关的基因表达减少和与炎症过程相关的基因表达增加。在非应答者中,T细胞无能的诱导,雄激素信号的正向调节,突触传递和囊泡运输以及应答者中细胞周期抑制和免疫应答的诱导也得到了丰富。我们鉴定了77个探针(54个基因)的表达特征,这些探针可预测100%病例的反应。他们中的五个能够在独立的数据集(P = 0.0056)上准确预测52例用来曲唑治疗的ER +乳腺癌的反应。来自阿那曲唑研究的十个固定的独立样品也用于RT-qPCR验证。这项研究表明,在治疗前的活检中分析的相对较少的基因可能会识别出可能对AI新辅助治疗有反应的患者。这可能具有可翻译为诊所的实用工具。此外,它描绘了对AI治疗具有内在抗性的新机制,可以对其进行进一步研究以探索规避治疗方法。

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