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首页> 外文期刊>Post?py Higieny i Medycyny Do?wiadczalnej >Molecular mechanisms of antitumor activity of taxanes. I. Interaction of docetaxel with microtubules
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Molecular mechanisms of antitumor activity of taxanes. I. Interaction of docetaxel with microtubules

机译:紫杉烷类抗肿瘤活性的分子机制。 I.多西紫杉醇与微管的相互作用

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Docetaxel (Taxotere), a new semisynthetic taxoid, is a mitotic inhibitor, widely used in monotherapy or in combination with other anticancer drugs against many types of cancer. The structure and dynamics of microtubules as the main target for docetaxel activity inside the cell and the taxane-binding site on β-tubulin are discussed. Microtubules are highly dynamic assemblies of α- and β-tubulin. They readily polymerize and depolymerize in cells and these dynamic behaviours are crucial to cell mitosis. Microtubule instability is attributed to their capability to hydrolyze GTP to GDP, which causes their depolymerization. Addition of new α-, β-tubulin heterodimer bound to GTP leads to tubulin polymerization, which increases the length of the microtubule. Docetaxel alters the polymerization dynamics of microtubules, which causes blockage of cell mitosis, and consequently induces apoptotic and non-apoptotic cell death. Docetaxel specifically acts on the S, M and G2 phases of the cell cycle. This paper reviews the current state of knowledge related to the molecular mechanisms of docetaxel action on the cell cycle and microtubule dynamics. In addition, a brief survey of the present state of research on the new generation (2nd and 3rd) of taxanes is presented.
机译:多西他赛(Taxotere)是一种新型的半合成紫杉烷,是一种有丝分裂抑制剂,广泛用于单一疗法或与其他抗癌药物联合使用,可对抗多种类型的癌症。讨论了作为细胞内多西他赛活性的主要靶标的微管的结构和动力学以及β-微管蛋白上的紫杉烷结合位点。微管是α-和β-微管蛋白的高度动态装配。它们容易在细胞中聚合和解聚,这些动态行为对细胞有丝分裂至关重要。微管的不稳定性归因于它们将GTP水解为GDP的能力,从而导致其解聚。与GTP结合的新的α-,β-微管蛋白异二聚体的添加导致微管蛋白聚合,从而增加了微管的长度。多西他赛改变了微管的聚合动力学,导致细胞有丝分裂受阻,并因此导致凋亡和非凋亡细胞死亡。多西紫杉醇特异性作用于细胞周期的S,M和G2期。本文回顾了有关多西他赛作用于细胞周期和微管动力学的分子机制的相关知识。另外,简要概述了新一代(第二和第三代)紫杉烷类的研究现状。

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