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首页> 外文期刊>Annals of Oncology >Understanding the biology of triple-negative breast cancer
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Understanding the biology of triple-negative breast cancer

机译:了解三阴性乳腺癌的生物学

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Greater understanding of the biology of triple-negative breast cancer (TNBC) is needed to discern the roughly 60% of node-negative patients who are already cured with locoregional therapy from the 40% who need adjuvant systemic therapy to be cured. Recent evidence suggests that patients with TNBC whose tumours have an activated immune response gene signature have a more favourable outcome than TNBC patients without this signature. For the group who needs additional systemic therapy, the challenge remains to choose the right systemic drug combination for the right TNBC sub-type. Significant heterogeneity exists within the TNBC class that is exemplified by differing chemotherapeutic sensitivity observed for some sub-types. This heterogeneity establishes the need for identifying differentiating molecular markers within the overall class of TNBC disease, which may help refine therapeutic management. In this review, we discuss some of these promising predictive molecular markers for tailoring therapy. In addition, several gene expression profiling and functional studies employing genetic screens that help to establish TNBC sub-groups with varying sensitivities to a variety of targeted therapies currently under clinical investigation are conferred. It is anticipated that a greater understanding of the biology of TNBC and its complex heterogeneity will reveal novel targets or identify markers around which clinical trials in molecularly well-defined sub-groups can be designed.
机译:需要对三阴性乳腺癌(TNBC)的生物学有更深入的了解,才能将大约60%的已经接受局部治疗治愈的淋巴结阴性患者和40%的需要进行全身辅助治疗的患者区分开。最近的证据表明,其肿瘤具有激活的免疫反应基因特征的TNBC患者比没有该特征的TNBC患者具有更好的预后。对于需要额外全身治疗的人群,挑战仍然是为正确的TNBC亚型选择正确的全身药物组合。 TNBC类内存在显着的异质性,这可以通过对某些亚型观察到的不同化学敏感性来证明。这种异质性导致需要在整个TNBC疾病类别中识别差异化分子标记,这可能有助于改善治疗管理。在这篇综述中,我们讨论了一些有前途的预测性分子标记物,用于定制疗法。另外,还提出了一些利用基因筛选的基因表达谱和功能研究,这些研究有助于建立对目前正在临床研究中的各种靶向疗法具有不同敏感性的TNBC亚组。预计对TNBC生物学及其复杂异质性的更多了解将揭示新的靶标或鉴定标志物,围绕这些目标物或分子标志物,可以设计在分子明确的亚组中进行临床试验。

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