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Revisiting ovarian cancer microenvironment: a friend or a foe?

机译:回顾卵巢癌微环境:是敌还是友?

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摘要

Development of ovarian cancer involves the co-evolution of neoplastic cells together with the adjacent microenvironment. Steps of malignant progression including primary tumor outgrowth, therapeutic resistance, and distant metastasis are not determined solely by genetic alterations in ovarian cancer cells, but considerably shaped by the fitness advantage conferred by benign components in the ovarian stroma. As the dynamic cancer topography varies drastically during disease progression, heterologous cell types within the tumor microenvironment (TME) can actively determine the pathological track of ovarian cancer. Resembling many other solid tumor types, ovarian malignancy is nurtured by a TME whose dark side may have been overlooked, rather than overestimated. Further, harnessing breakthrough and targeting cures in human ovarian cancer requires insightful understanding of the merits and drawbacks of current treatment modalities, which mainly target transformed cells. Thus, designing novel and precise strategies that both eliminate cancer cells and manipulate the TME is increasingly recognized as a rational avenue to improve therapeutic outcome and prevent disease deterioration of ovarian cancer patients.
机译:卵巢癌的发展涉及肿瘤细胞与邻近微环境的共同进化。恶性进展的步骤,包括原发肿瘤的长大,治疗抗性和远处转移,不仅取决于卵巢癌细胞的遗传改变,而且还取决于卵巢基质中良性成分的适应性优势。由于动态癌症的地形在疾病发展过程中发生巨大变化,因此肿瘤微环境(TME)中的异源细胞类型可以主动确定卵巢癌的病理轨迹。与许多其他实体瘤类型类似,TME会滋生卵巢恶性肿瘤,其阴暗面可能已被忽视,而不是被高估了。此外,在人类卵巢癌中利用突破性疗法和靶向疗法需要深入了解当前治疗方法的优缺点,这些治疗方法主要靶向转化细胞。因此,越来越多地设计出既消除癌细胞又控制TME的新颖精确策略,已成为改善治疗效果和预防卵巢癌患者疾病恶化的合理途径。

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