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Triple-negative breast cancer: Molecular subtypes and targeted therapy

机译:三阴性乳腺癌:分子亚型和靶向治疗

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PURPOSE OF REVIEW: Triple-negative breast cancers (TNBCs), lacking estrogen receptor expression and human epidermal growth factor receptor 2 amplification, have no effective targeted therapy. Large-scale comprehensive genomic analyses have allowed stratification of TNBCs by molecular features. We will review the recent data regarding the classification of these poor prognosis cancers and the associated potential targeted treatment approaches. RECENT FINDINGS: TNBCs are a heterogeneous set of cancers characterized by a diverse set of gene-expression patterns and underlying genomic changes. Mutations in p53 are the only genomic alteration present in the majority of TNBCs. Other potential targetable alterations are only present in small subsets of TNBCs, and include defects in DNA repair present in BRCA1-mutant TNBCs and some sporadic TNBCs. Antiandrogens may be effective for TNBCs that express the androgen receptor and have luminal-like gene-expression features. PI3KCA pathway inhibitors and HSP90 inhibitors may also be effective in a small fraction of TNBCs. SUMMARY: Robust methods to functionally classify TNBCs to determine vulnerable pathways are urgently needed to guide the development of clinical trials. It is quite possible that TNBCs, like non-small cell lung cancer, will be stratified into many individually rare cancer classes, each requiring a distinct treatment approach.
机译:审查目的:缺乏雌激素受体表达和人类表皮生长因子受体2扩增的三阴性乳腺癌(TNBCs)没有有效的靶向治疗。大规模的全面基因组分析已允许通过分子特征对TNBCs进行分层。我们将回顾有关这些预后不良癌症的分类以及相关的潜在靶向治疗方法的最新数据。最近的发现:TNBC是一组异质性癌症,其特征是具有多种基因表达模式和潜在的基因组变化。 p53中的突变是大多数TNBC中存在的唯一基因组改变。其他潜在的可靶向改变仅存在于一小部分的TNBC中,包括BRCA1突变的TNBC和一些零星TNBC中存在的DNA修复缺陷。抗雄激素可能对表达雄激素受体并具有腔样基因表达功能的TNBC有效。 PI3KCA途径抑制剂和HSP90抑制剂在一小部分TNBC中也可能有效。简介:迫切需要可靠的方法来对TNBCs进行功能分类以确定易受感染的途径,以指导临床试验的发展。像非小细胞肺癌一样,TNBC很可能会被分为许多单独的罕见癌症类别,每种类别都需要不同的治疗方法。

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