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Bim-targeted cancer therapy: a link between drug action and underlying molecular changes.

机译:针对Bim的癌症疗法:药物作用与潜在分子变化之间的联系。

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摘要

In the past few years, the pro-apoptotic molecule Bim has attracted increasing attention as a plausible target for tumor therapy. A variety of normal and pathological systems regulated by Bim, dependent on cell type, apoptotic stimulation, and chemotherapeutic agents, have been documented. Bim promotes anoikis of many tumor cells, such as lung cancer, breast cancer, osteosarcoma, and melanoma. Various chemotherapeutic agents use Bim as a mediating executioner of cell death. Hence, Bim suppression supports metastasis and chemoresistance. Imatinib, gefitinib, bortezomib, and Bim protein itself are spotlighted as current and future Bim-targeting therapeutic agents. The potential benefits of Bim-targeted therapies are selectivity of treatment for tumor cells and reduction in tumor-associated phenomena such as chemoresistance and metastasis. Thus, Bim-targeting therapies may provide more effective and unique tumor management modalities in future. This review article discusses all these issues.
机译:在过去的几年中,促凋亡分子Bim作为肿瘤治疗的合理靶点已引起越来越多的关注。已经证明了多种受Bim调节的正常和病理系统,具体取决于细胞类型,凋亡刺激和化学治疗剂。 Bim促进许多肿瘤细胞的无神经,例如肺癌,乳腺癌,骨肉瘤和黑色素瘤。多种化学治疗剂使用Bim作为细胞死亡的中介执行者。因此,Bim抑制支持转移和化学耐药性。伊马替尼,吉非替尼,硼替佐米和Bim蛋白本身已成为当前和未来针对Bim的治疗剂。 Bim靶向疗法的潜在好处是对肿瘤细胞的选择性治疗以及减少与肿瘤相关的现象(例如化学抗性和转移性)。因此,Bim靶向疗法可能会在将来提供更有效和独特的肿瘤治疗方式。这篇评论文章讨论了所有这些问题。

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