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The γ-tubulin-specific inhibitor gatastatin reveals temporal requirements of microtubule nucleation during the cell cycle

机译:γ-微管蛋白特异性抑制剂加他汀对细胞周期中微管成核的时间要求

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Inhibitors of microtubule (MT) assembly or dynamics that target α/β-tubulin are widely exploited in cancer therapy and biological research. However, specific inhibitors of the MT nucleator γ-tubulin that would allow testing temporal functions of γ-tubulin during the cell cycle are yet to be identified. By evolving β-tubulin-binding drugs we now find that the glaziovianin A derivative gatastatin is a γ-tubulin-specific inhibitor. Gatastatin decreased interphase MT dynamics of human cells without affecting MT number. Gatastatin inhibited assembly of the mitotic spindle in prometaphase. Addition of gatastatin to preformed metaphase spindles altered MT dynamics, reduced the number of growing MTs and shortened spindle length. Furthermore, gatastatin prolonged anaphase duration by affecting anaphase spindle structure, indicating the continuous requirement of MT nucleation during mitosis. Thus, gatastatin facilitates the dissection of the role of γ-tubulin during the cell cycle and reveals the sustained role of γ-tubulin.
机译:针对α/β-微管蛋白的微管(MT)组装或动力学抑制剂在癌症治疗和生物学研究中得到了广泛利用。然而,尚未确定MT成核剂γ-微管蛋白的特异性抑制剂,其可在细胞周期中测试γ-微管蛋白的时间功能。通过发展与β-微管蛋白结合的药物,我们现在发现glaziovianin A衍生物加他他汀是一种γ-微管蛋白特异性抑制剂。加他汀抑制人细胞间期MT动态,而不影响MT数量。加他汀抑制前中期的有丝分裂纺锤体的组装。向预制的中期纺锤体中添加加他汀可改变MT动态,减少MT生长数量并缩短纺锤体长度。此外,加他他汀通过影响后期纺锤体结构延长了后期持续时间,表明在有丝分裂期间对MT成核的持续需求。因此,加他汀可促进细胞周期中γ-微管蛋白的作用分离,并揭示γ-微管蛋白的持续作用。

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