Drug design and discovery最新文献

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QSAR of antineoplastics IV: Hansch analysis of N-(7-indolyl)benzenesulfonamides against KB human nasopharynx carcinoma, colon 38 murine adenocarcinoma and P388 murine leukemia cell lines. 抗肿瘤药物的 QSAR IV：N-(7-吲哚基)苯磺酰胺类药物对 KB 人鼻咽癌、结肠 38 小鼠腺癌和 P388 小鼠白血病细胞系的 Hansch 分析。

Drug design and discovery

Pub Date : 2001-01-01

K Roy, D K Pal, A U De, C Sengupta

Hansch analysis of recently reported antitumor activities of novel N-(7-indolyl)benzenesulfonamide derivatives against KB human nasopharynx carcinoma, colon 38 murine adenocarcinoma and P388 murine leukemia cell lines reveals that the pattern of receptor interactions in human KB cells differs from that in murine (colon 38 and P388 leukemia) cells. The latter two activities are autocorrelated and show similar receptor specificity. It seems that two binding sites, one interacting with the indole fragment and another with phenyl fragment of the indolylbenzenesulfonamide compounds, are present on the murine cell receptors (colon 38 and P388 leukemia) while only the latter binding site is active on the human KB cell receptors. For the activity against KB cells, a para-methyl or paramethoxy substituent on the phenyl ring of benzenesulfonamide moiety greatly enhances the activity. For the other two activities, a 3-chloro or 3-cyano substituent on indole nucleus enhances activities, while presence of bulkier meta or para substituent on the phenyl ring decreases activities. Presence of an ortho substituent on the phenyl ring appears to be detrimental for all the three activities. Equations generated by both QSAR and QAAR studies are quite robust as evidenced from cross-validation by 'leave-one-out' technique.

对最近报道的新型 N-(7-吲哚基)苯磺酰胺衍生物对人类 KB 鼻咽癌、小鼠 38 号结肠腺癌和 P388 小鼠白血病细胞系的抗肿瘤活性进行的 Hansch 分析表明，人类 KB 细胞与小鼠（38 号结肠腺癌和 P388 白血病）细胞的受体相互作用模式不同。后两种活性是自相关的，并显示出类似的受体特异性。在小鼠细胞受体（结肠 38 和 P388 白血病）上似乎存在两个结合位点，一个与吲哚片段相互作用，另一个与吲哚苯磺酰胺化合物的苯基片段相互作用，而在人类 KB 细胞受体上只有后一个结合位点具有活性。就对 KB 细胞的活性而言，苯磺酰胺分子苯环上的对甲氧基或对甲氧基取代基可大大提高其活性。就其他两种活性而言，吲哚核上的 3-氯或 3-氰基取代基会增强活性，而苯环上较大的元或对位取代基则会降低活性。苯环上的正交取代基似乎对所有三种活性都不利。QSAR 和 QAAR 研究得出的方程都相当稳健，这一点可以通过 "留一剔除 "技术进行交叉验证得到证明。

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引用次数: 0

QSAR of antineoplastics V: Exploration of receptor interaction sites of antitumor N-(7-indolyl)benzenesulfonamides targeting GI phase using electrotopological state atom index. 抗肿瘤药物的 QSAR V：利用电拓态原子指数探索以 GI 相为目标的 N-(7-吲哚基)苯磺酰胺类抗肿瘤药物的受体相互作用位点。

Drug design and discovery

Pub Date : 2001-01-01

K Roy, D K Pal, C Sengupta

Quantitative structure activity relationship (QSAR) study of antiproliferative activities of N-(7-indolyl)benzenesulfonamides with electrotopological state atom (ETSA) index corroborates the conclusions of the previously reported Hansch analysis that the structural requirements for interactions with receptors of human KB nasopharynx cell line are different from that for murine colon 38 and P388 leukemia cell lines. The study suggests that both phenyl ring and indole moiety are the important receptor interaction sites present on the ligands for the murine cell lines, while the latter site does not appear to play significant role in case of human KB cell carcinoma.

用电拓扑状态原子（ETSA）指数对 N-(7-吲哚基)苯磺酰胺类化合物的抗增殖活性进行的定量结构活性关系（QSAR）研究证实了之前报道的 Hansch 分析得出的结论，即与人类 KB 鼻咽细胞系受体相互作用的结构要求不同于鼠结肠 38 和 P388 白血病细胞系。研究表明，对于小鼠细胞系来说，配体上的苯环和吲哚分子都是重要的受体相互作用位点，而对于人类 KB 细胞癌来说，后一个位点似乎不起重要作用。

引用次数: 0

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