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Paclitaxel-Conjugated PAMAM Dendrimers Adversely Affect Microtubule Structure through Two Independent Modes of Action

机译:紫杉醇偶联的PAMAM树状聚合物通过两种独立的作用方式不利地影响微管结构。

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摘要

Paclitaxel (Taxol) is an anticancer drug that induces mitotic arrest via microtubule hyperstabilization but causes side effects due to its hydrophobicity and cellular promiscuity. The targeted cytotoxicity of hydrophilic paclitax-el-conjugated polyamidoamine (PAMAM) dendrimers has been demonstrated in cultured cancer cells. Mechanisms of action responsible for this cytotoxicity are unknown, that is, whether the cytotoxicity is due to paclitaxel stabilization of microtubules, as is whether paclitaxel is released intracellularly from the dendrimer. To determine whether the conjugated paclitaxel can bind microtubules, we used a combination of ensemble and single microtubule imaging techniques in vitro. We demonstrate that these conjugates adversely affect microtubules by (1) promoting the polymerization and stabilization of microtubules in a paclitaxel-dependent manner, and (2) bundling preformed microtubules in a paclitaxel-independent manner, potentially due to protonation of tertiary amines in the dendrimer interior. Our results provide mechanistic insights into the cytotoxicity of paclitaxel-conjugated PAMAM dendrimers and uncover unexpected risks of using such conjugates therapeutically.
机译:紫杉醇(Taxol)是一种抗癌药物,可通过微管超稳定作用诱导有丝分裂停滞,但由于其疏水性和细胞混杂性而引起副作用。已在培养的癌细胞中证明了亲水性紫杉醇-el共轭聚酰胺型(PAMAM)树状聚合物的靶向细胞毒性。造成这种细胞毒性的作用机理尚不清楚,也就是说,细胞毒性是否是由于紫杉醇稳定了微管,还是因为紫杉醇是否从树状大分子中释放出来。为了确定共轭紫杉醇是否可以结合微管,我们在体外使用了集成和单个微管成像技术的组合。我们证明这些共轭物通过(1)以紫杉醇依赖性的方式促进微管的聚合和稳定化,以及(2)以紫杉醇非依赖性的方式捆绑预制微管,可能对树枝状大分子中的叔胺质子化产生不利影响室内。我们的结果提供了对紫杉醇缀合的PAMAM树状聚合物的细胞毒性的机械见解,并揭示了治疗性使用此类缀合物的意外风险。

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