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Application of ProTide technology to gemcitabine: A successful approach to overcome the key cancer resistance mechanisms leads to a new agent (NUC-1031) in clinical development

机译:ProTide技术在吉西他滨的应用:克服关键抗癌机制的成功方法导致了临床开发中的新药(NUC-1031)

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摘要

Gemcitabine is a nucleoside analogue commonly used in cancer therapy but with limited efficacy due to a high susceptibility to cancer cell resistance. The addition of a phosphoramidate motif to the gemcitabine can protect it against many of the key cancer resistance mechanisms. We have synthesized a series of gemcitabine phosphoramidate prodrugs and screened for cytostatic activity in a range of different tumor cell lines. Among the synthesized compounds, one in particular (NUC-1031, 6f) was shown to be potent in vitro. Importantly, compared with gemcitabine, 6f activation was significantly less dependent on deoxycytidine kinase and on nucleoside transporters, and it was resistant to cytidine deaminase-mediated degradation. Moreover, 6f showed a significant reduction in tumor volumes in vivo in pancreatic cancer xenografts. The ProTide 6f is now in clinical development with encouraging efficacy signals in a Phase I/II study, which strongly supports the ProTide approach to generate promising new anticancer agents.
机译:吉西他滨是一种常用于癌症治疗的核苷类似物,但由于对癌细胞耐药的敏感性较高,因此疗效有限。在吉西他滨中添加氨基磷酸酯基序可以使其免受许多关键的抗癌机制影响。我们合成了一系列吉西他滨氨基磷酸酯前药,并筛选了一系列不同肿瘤细胞系中的细胞抑制活性。在合成的化合物中,特别是一种化合物(NUC-1031,6f)在体外表现出强效作用。重要的是,与吉西他滨相比,6f激活对脱氧胞苷激酶和核苷转运蛋白的依赖性显着降低,并且对胞苷脱氨酶介导的降解具有抗性。此外,在胰腺癌异种移植物中,6f显示体内肿瘤体积显着减少。 ProTide 6f目前正在临床开发中,在I / II期研究中具有令人鼓舞的功效信号,该研究强烈支持ProTide方法产生有希望的新抗癌药。

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