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Therapeutic Advances and New Directions for Triple-Negative Breast Cancer

机译:三阴性乳腺癌的治疗进展和新方向

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Triple-negative breast cancer (TNBC) is a molecularly diverse grouping with poor prognosis for which chemotherapy remains the foundation of treatment. The molecular heterogeneity of the disease rationalizes its diverse biological behavior and differential response to treatment. Estimates of up to 20% of patients diagnosed have germline mutations in DNA-damage repair-pathway genes, namely BRCA1 and 2, and this can be used to select patients likely to respond to platinums and/or inhibitors of poly(ADP-ribose) polymerase (PARP). Similar strategies can be utilized in other subtypes of TNBC that have ‘BRCA-like’ tumor biology due to the presence of mutations in alternate DNA-damage repair genes. The diverse biological behavior of TNBC and its variable response to chemotherapy were largely decoded following genotyping studies that enabled the identification of distinct molecular subtypes, such that the biological and genetic heterogeneity of the disease could be understood. This subsequently enabled the identification of therapeutic ‘vulnerabilities’ for each subtype that encompass biological processes including proliferation, DNA repair, apoptosis, angiogenesis, immune modulation, and invasion and metastasis. To expedite the development of therapies for high-risk, early-stage breast cancer, we have adopted novel trial designs and re-defined endpoints as surrogates of clinical outcomes. The purpose of this review is to highlight the current standard and experimental treatment options for TNBC.
机译:三阴性乳腺癌(TNBC)是一个分子多样性高,预后差的组,化疗仍是治疗的基础。该疾病的分子异质性合理化了其多种生物学行为和对治疗的不同反应。估计多达20%的被诊断患有DNA损伤修复途径基因即BRCA1和2的种系突变的患者,可用于选择可能对铂和/或多聚(ADP-核糖)抑制剂有反应的患者聚合酶(PARP)。由于其他DNA损伤修复基因中存在突变,因此类似的策略也可用于具有“ BRCA样”肿瘤生物学特性的TNBC其他亚型。在基因分型研究之后,TNBC的多种生物学行为及其对化学疗法的可变反应在很大程度上得以解码,这使得能够鉴定出不同的分子亚型,从而可以理解该疾病的生物学和遗传异质性。随后,这为每种亚型确定了治疗性“弱点”,涵盖了生物学过程,包括增殖,DNA修复,凋亡,血管生成,免疫调节以及侵袭和转移。为了加快开发高危早期乳腺癌的治疗方法,我们采用了新颖的试验设计并重新定义了终点指标,作为临床疗效的替代指标。这篇综述的目的是强调TNBC的当前标准和实验治疗方案。

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