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Epigenetic and Pluripotency Aspects of Disseminated Cancer Cells During Minimal Residual Disease

机译:在最小残留疾病中播散癌细胞的表观遗传和多能性方面

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Our understanding of the minimal residual disease (MRD) in solid cancers indicates that it can persist in the system for years or even decades. We now know that the persistence of MRD might depend on the dormancy of the disseminated cancer cells (DCCs). Once DCCs exit dormancy, they become metastatic and the survival rates of the patients inevitably decrease. Thus, innovative treatments are required to extend the asymptomatic phase of MRD after the initial therapeutic intervention. With the latest advances in cancer research, there is a greater need to explore and understand the biology, timing of dissemination, and origin of DCCs during tumor progression. These important aspects of DCCs impact the selection, design, administration, and timing of effective therapies. Herein, we summarize the current understanding of MRD biology in solid tumors, with a focus on epigenetics and pluripotency, presenting an overall view of the direction the field is taking to reach the goal of reducing cancer-related mortalities that result from metastasis.
机译:我们对固体癌症中最小的残留疾病(MRD)的理解表明它可以在系统中持续多年甚至数十年。我们现在知道MRD的持久性可能取决于播散癌细胞(DCCS)的休眠。一旦DCC出出休眠,它们就会成为转移性的,并且患者的存活率不可避免地减少。因此,需要在初始治疗干预后延长MRD的无症状阶段。随着癌症研究的最新进展,在肿瘤进展期间,探讨和理解DCCS的生物学,时序以及DCCS的起源。 DCC的这些重要方面会影响有效疗法的选择,设计,管理和时序。在此,我们总结了目前对实体肿瘤的MRD生物学的认识,重点是表观遗传和多能性,展示了该领域的方向,以达到降低转移导致的癌症相关的死亡率的目标。

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