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Chemotherapeutic Potential of Diazeniumdiolate-based Aspirin Prodrugs in Breast Cancer

机译:基于二醇二氮烯鎓的阿司匹林前药的化学治疗潜力

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摘要

Diazeniumdiolate-based aspirin prodrugs have previously been shown to retain the anti-inflammatory properties of aspirin while protecting against the common side effect of stomach ulceration. Initial analysis of two new prodrugs of aspirin that also release either nitroxyl (HNO) or nitric oxide (NO) demonstrated increased cytotoxicity toward human lung carcinoma cells compared to either aspirin or the parent nitrogen oxide donor. In addition, cytotoxicity was significantly lower in endothelial cells, suggesting cancer-specific sensitivity. To assess the chemotherapeutic potential of these new prodrugs in breast cancer, we studied their effect both in cultured cells and in a nude mouse model. Both prodrugs reduced growth of breast adenocarcinoma cells more effectively than the parent compounds while not being appreciably cytotoxic in a related non-tumorigenic cell line (MCF-10A). The HNO donor also was more cytotoxic than the related NO donor. The basis for the observed specificity was investigated in terms of impact on metabolism, DNA damage and repair, apoptosis, angiogenesis and metastasis. The results suggest a significant pharmacological potential for treatment of breast cancer.
机译:先前已显示出基于二氮杂二氮杂酸酯的阿司匹林前药保留了阿司匹林的抗炎特性,同时防止胃溃疡的常见副作用。对两种新的阿司匹林前药的初步分析表明,与阿司匹林或母体一氧化氮供体相比,阿司匹林的两种前药也能释放出硝酰基(HNO)或一氧化氮(NO)。另外,内皮细胞的细胞毒性显着降低,表明癌症特异性敏感性。为了评估这些新药在乳腺癌中的化学治疗潜力,我们研究了它们在培养细胞和裸鼠模型中的作用。两种前药均比母体化合物更有效地减少了乳腺癌细胞的生长,同时在相关的非致瘤细胞系(MCF-10A)中没有明显的细胞毒性。 HNO供体也比相关的NO供体具有更高的细胞毒性。从对代谢,DNA损伤和修复,细胞凋亡,血管生成和转移的影响方面研究了观察到的特异性的基础。结果表明治疗乳腺癌的重要药理潜力。

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