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Prediction of breast cancer metastasis by genomic profiling: where do we stand?

机译:通过基因组分布图预测乳腺癌转移:我们站在哪里?

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摘要

Current concepts conceive “breast cancer” as a complex disease that comprises several very different types of neoplasms. Nonetheless, breast cancer treatment has considerably improved through early diagnosis, adjuvant chemotherapy, and endocrine treatments. The limited prognostic power of classical classifiers determines considerable over-treatment of women who either do not benefit from, or do not at all need, chemotherapy. Several gene expression based molecular classifiers (signatures) have been developed for a more reliable prognostication. Gene expression profiling identifies profound differences in breast cancers, most probably as a consequence of different cellular origin and different driving mutations and can therefore distinguish the intrinsic propensity to metastasize. Existing signatures have been shown to be useful for treatment decisions, although they have been developed using relatively small sample numbers. Major improvements are expected from the use of large datasets, subtype specific signatures and from the re-introduction of functional information. We show that molecular signatures encounter clear limitations given by the intrinsic probabilistic nature of breast cancer metastasis. Already today, signatures are, however, useful for clinical decisions in specific cases, in particular if the personal inclination of the patient towards different treatment strategies is taken into account.
机译:当前的概念将“乳腺癌”视为一种复杂的疾病,包括几种非常不同类型的肿瘤。尽管如此,通过早期诊断,辅助化学疗法和内分泌治疗,乳腺癌的治疗已大大改善。经典分类器的预后能力有限,决定了无法从化疗中获益或根本不需要化疗的女性过度治疗的情况。已经开发了几种基于基因表达的分子分类器(签名)以实现更可靠的预后。基因表达谱分析发现了乳腺癌的深远差异,这很可能是由于不同的细胞起源和不同的驱动突变导致的,因此可以区分内在的转移倾向。尽管已经使用相对较小的样本数量开发了现有签名,但已证明它们对治疗决策很有用。预期将通过使用大型数据集,特定于子类型的签名以及重新引入功能信息来取得重大改进。我们表明,分子标志遇到乳腺癌转移的内在概率性质所赋予的明显局限性。但是,如今,签名已可用于特定情况下的临床决策,尤其是考虑到患者对不同治疗策略的个人倾向时。

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