Cytotoxicity and topo I targeting activity of substituted 10--nitrogenous heterocyclic aromatic group derivatives of SN-38.

Li QY; Deng XQ; Zu YG; Lv H; Su L; Yao L; Zhang Y; Li L

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Cytotoxicity and topo I targeting activity of substituted 10--nitrogenous heterocyclic aromatic group derivatives of SN-38.

机译：SN-38取代的10-氮杂环芳香族衍生物的细胞毒性和topo I靶向活性。

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A series of 10-position substituted nitrogenous heterocyclic aromatic group derivatives of SN-38 were prepared. Most of these compounds possessed lower cytotoxicities than CPT. Compound 13 revealed potent cytotoxicity similar to CPT, and compounds 17, 18, and 19 showed similar cytotoxic activity to topotecan. All of the pyridine salt derivatives (7-16) revealed comparable or superior topo I inhibitory activity in relation to CPT. Ethyl in the 7-position of these compounds can increase the cytotoxicity and inhibitory activity to topo I compared with corresponding pyridine salts CPT derivatives (7a-13a) and simultaneously maintain good water solubility. This result is consistent with the SAR of CPT.

机译：制备了一系列的SN-38的10位取代的含氮杂环芳族衍生物。这些化合物大多数具有比CPT低的细胞毒性。化合物13显示出与CPT相似的有效细胞毒性，而化合物17、18和19显示出与拓扑替康相似的细胞毒性活性。所有吡啶盐衍生物（7-16）均显示出与CPT相当或更好的topo I抑制活性。与相应的吡啶盐CPT衍生物（7a-13a）相比，这些化合物7位上的乙基可以增加对topo I的细胞毒性和抑制活性，并同时保持良好的水溶性。此结果与CPT的SAR一致。

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《European Journal of Medicinal Chemistry: Chimie Therapeutique》 |2010年第7期|共7页
作者
Li QY; Deng XQ; Zu YG; Lv H; Su L; Yao L; Zhang Y; Li L;
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正文语种 eng
中图分类医药、卫生;劳动卫生;
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机译：SN-38取代的10-氮杂环芳香族衍生物的细胞毒性和topo I靶向活性。
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Cytotoxicity and topo I targeting activity of substituted 10--nitrogenous heterocyclic aromatic group derivatives of SN-38.

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