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Targeted therapy of epigenomic regulatory mechanisms controlling the epithelial to mesenchymal transition during tumor progression

机译:在肿瘤进展过程中控制上皮向间质转化的表观基因调控机制的靶向治疗

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摘要

The epithelial-to-mesenchymal transition (EMT) is a reversible change in cell phenotype that plays a crucial role during normal development and cancer metastasis. EMT imparts embryonic epithelial cells with the ability to migrate and to give rise to organs or tissues at distant sites. During cancer progression, the same developmental process is utilized in an analogous manner to enable cancer cells to move to distant organs and form metastases. The reversion of EMT via the mesenchymal-to-epithelial transition (MET) appears to be required for the formation of secondary tumors at distal sites. The plasticity of epigenomic modifications that control the transcriptional program of cells enables cells to switch back and forth from epithelial and mesenchymal phenotypes during these transitions. Here, we review the interplay between complex epigenomic regulatory mechanisms and various transcription factors involved in EMT leading to changes in gene expression and cell phenotype. We also discuss the way that a deeper understanding of the epigenomic regulation of EMT might shed light onto the process of cancer progression and reveal new targets for novel and more specific anticancer epigenomic therapies.
机译:上皮到间质转化(EMT)是细胞表型的可逆变化,在正常发育和癌症转移过程中起着至关重要的作用。 EMT使胚胎上皮细胞具有迁移能力并在远处产生器官或组织。在癌症进展期间,以类似的方式利用相同的发育过程,以使癌细胞能够移动到远处的器官并形成转移灶。通过间质到上皮的转变(MET)逆转EMT似乎是在远端部位形成继发性肿瘤所必需的。控制细胞转录程序的表观基因组修饰的可塑性使细胞能够在这些过渡过程中从上皮和间充质表型来回切换。在这里,我们审查复杂的基因组调控机制和EMT中涉及导致基因表达和细胞表型变化的各种转录因子之间的相互作用。我们还讨论了对EMT的表观基因组调控更深入的了解可能会揭示癌症进展过程并揭示新颖且更具体的抗癌表观基因组治疗新靶标的方式。

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