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Mechanisms of disseminated cancer cell dormancy: an awakening field

机译:癌细胞扩散的休眠机制:一个觉醒的领域

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Metastases arise from residual disseminated tumour cells (DTCs). This can happen years after primary tumour treatment because residual tumour cells can enter dormancy and evade therapies. As the biology of minimal residual disease seems to diverge from that of proliferative lesions, understanding the underpinnings of this new cancer biology is key to prevent metastasis. Analysis of approximately 7 years of literature reveals a growing focus on tumour and normal stem cell quiescence, extracellular and stromal microenvironments, autophagy and epigenetics as mechanisms that dictate tumour cell dormancy. In this Review, we attempt to integrate this information and highlight both the weaknesses and the strengths in the field to provide a framework to understand and target this crucial step in cancer progression.
机译:转移来自残余的播散性肿瘤细胞(DTC)。这可能在原发肿瘤治疗后数年发生,因为残留的肿瘤细胞可以进入休眠状态并逃避治疗。由于最小残留疾病的生物学似乎与增生性病变的生物学不同,因此了解这种新的癌症生物学的基础是预防转移的关键。对大约7年文献的分析表明,人们越来越关注肿瘤和正常干细胞的静止,细胞外和基质微环境,自噬和表观遗传学,这些机制决定了肿瘤细胞的休眠状态。在本综述中,我们试图整合这些信息,并强调该领域的弱点和优势,以提供一个框架来理解和靶向癌症进展中的这一关键步骤。

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