对P388白血病细胞具有高活性的3,5-双苄基-4-哌啶酮及其相关化合物。

Drug design and delivery Pub Date : 1990-09-01
J R Dimmock, V K Arora, S L Wonko, N W Hamon, J W Quail, Z Jia, R C Warrington, W D Fang, J S Lee
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引用次数: 0

摘要

制备了3,5-双(苄基)-4-哌啶酮及其相关化合物,发现其对P388白血病细胞的活性是N,N'-双(2-氯乙基)-N-亚硝基脲的100 ~ 9700倍。通过x射线晶体学测定了其中六种分子的形状,进行了比较,但分子的立体化学或电子性质与细胞毒性之间没有明显的相关性。通过形成两个单苄基化合物、一个相关的无环衍生物和一个n -酰基化合物的分子修饰,化合物的细胞毒性降低,但仍保持较高的细胞毒性。两种具有代表性的化合物在小鼠腹腔注射后降低了肝脏的谷胱甘肽水平。两种季铵化合物在DNA的小凹槽中结合,而四种相关的非季铵衍生物没有表现出这种性质。我们得出结论,这些高细胞毒性化合物的作用模式包括细胞硫醇的烷基化和DNA结合,但也可能涉及其他生化过程的干扰。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
3,5-Bis-benzylidene-4-piperidones and related compounds with high activity towards P388 leukemia cells.

3,5-Bis(benzylidene)-4-piperidones and related compounds were prepared and found to have between 100 and 9700 times the activity of N,N'-bis(2-chloroethyl)-N-nitrosourea towards P388 leukemia cells. The shapes of six of these molecules--determined by X-ray crystallography--were compared, but no correlation between the stereochemistry of the molecules or their electronic properties and cytotoxicity was apparent. Molecular modification of the compounds by forming two mono-benzylidene compounds, a related acyclic derivative and an N-acyl compound resulted in diminished but retained high cytotoxicity. Two representative compounds lowered glutathione levels of liver following their intraperitoneal injection into mice. Two quaternary ammonium compounds were shown to bind in the minor groove of DNA, while four related non-quaternary ammonium derivatives did not demonstrate this property. We conclude that the modes of action of these highly cytotoxic compounds include alkylation of cellular thiols and DNA binding, but interference with other biochemical processes is also probably involved.

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