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Learning about the Importance of Mutation Prevention from Curable Cancers and Benign Tumors

机译:学习突变预防可治愈癌症和良性肿瘤的重要性

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Some cancers can be cured by chemotherapy or radiotherapy, presumably because they are derived from those cell types that not only can die easily but also have already been equipped with mobility and adaptability, which would later allow the cancers to metastasize without the acquisition of additional mutations. From a viewpoint of biological dispersal, invasive and metastatic cells may, among other possibilities, have been initial losers in the competition for resources with other cancer cells in the same primary tumor and thus have had to look for new habitats in order to survive. If this is really the case, manipulation of their ecosystems, such as by slightly ameliorating their hardship, may prevent metastasis. Since new mutations may occur, especially during and after therapy, to drive progression of cancer cells to metastasis and therapy-resistance, preventing new mutations from occurring should be a key principle for the development of new anticancer drugs. Such new drugs should be able to kill cancer cells very quickly without leaving the surviving cells enough time to develop new mutations and select resistant or metastatic clones. This principle questions the traditional use and the future development of genotoxic drugs for cancer therapy.
机译:一些癌症可以通过化疗或放射治疗来治愈,这可能是因为它们来自那些不仅可以容易死亡而且还已经配备了迁移率和适应性的那些细胞类型,这将在不收购额外突变的情况下允许癌症转移。从生物分散的观点来看,侵入性和转移细胞可能在其他可能性中,在同一原发性肿瘤中与其他癌细胞的资源竞争是初始输家,因此必须寻找新的栖息地以便生存。如果真的是这种情况,他们的生态系统的操纵,例如通过稍微改善他们的困难,可能会阻止转移。由于可能发生新的突变,特别是在治疗期间和治疗期间,以推动癌细胞进展到转移和治疗抗性,防止发生的新突变应该是新抗癌药物发展的关键原则。这种新药应该能够非常快速地杀死癌细胞而不留下存活的细胞足够的时间开发新的突变并选择抗性或转移性克隆。这个原则问题是传统的使用和未来发展癌症治疗的遗传毒性药物。

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