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Genetic Dissection of Cancer Development, Therapy Response, and Resistance in Mouse Models of Breast Cancer.

机译:乳腺癌小鼠模型中癌症发展,治疗反应和耐药性的遗传解剖。

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摘要

The cancer genomics revolution has rapidly expanded the inventory of somatic mutations characterizing human malignancies, highlighting a previously underappreciated extent of molecular variability between and within patients. Also in breast cancer, the most commonly diagnosed malignancy in women, this heterogeneity complicates the understanding of the stepwise sequence of pathogenic events and the design of effective and long-lasting target therapies. To disentangle this complexity and pinpoint which molecular perturbations are crucial to hijack the cellular machinery and lead to tumorigenesis and drug resistance, functional studies are needed in model systems that faithfully and comprehensively recapitulate all the salient aspects of their cognate human counterparts. Mouse models of breast cancer have been instrumental for the study of tumor initiation and drug response but also involve cost and time limitations that represent serious bottlenecks in translational research. To keep pace with the overwhelming amount of hypotheses that warrant in vivo testing, continuous refinement of current breast cancer models and implementation of new technologies is crucial. In this review, we summarize the current state of the art in modeling human breast cancer in mice, and we put forward our vision for future developments.
机译:癌症基因组学革命迅速扩大了表征人类恶性肿瘤的体细胞突变的存量,突显了患者之间和患者内部分子变异性的先前未得到充分认识的程度。同样在乳腺癌中(女性最常被诊断为恶性肿瘤),这种异质性使对致病事件逐步序列的理解以及有效且持久的目标疗法的设计变得复杂。为了弄清这种复杂性并指出哪些分子扰动对于劫持细胞机制并导致肿瘤发生和耐药性至关重要,在模型系统中需要进行功能研究,以忠实和全面地概括其同类人类同行的所有重要方面。乳腺癌的小鼠模型对于研究肿瘤的发生和药物反应具有重要作用,但也存在成本和时间限制,这在转化研究中是严重的瓶颈。为了跟上需要进行体内测试的绝大多数假设,与时俱进,不断完善当前的乳腺癌模型和实施新技术至关重要。在这篇综述中,我们总结了在小鼠中对人类乳腺癌进行建模的最新技术,并提出了对未来发展的愿景。

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