植物生物碱新cryptolepine的DNA嵌入、拓扑异构酶II抑制及细胞毒活性。

Anti-cancer drug design Pub Date : 2000-06-01
C Bailly, W Laine, B Baldeyrou, M C De Pauw-Gillet, P Colson, C Houssier, K Cimanga, S Van Miert, A J Vlietinck, L Pieters
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引用次数: 0

摘要

隐tolepine和新隐tolepine是从非洲植物Cryptolepis sanguinolenta的根中分离出来的两种吲哚喹啉生物碱。这两种药物都显示出抗菌和抗寄生虫活性,并对肿瘤细胞具有很强的细胞毒性。我们最近的研究表明,隐tolepine可以嵌入到DNA中,并通过人类拓扑异构酶II刺激DNA切割。在这项研究中,我们研究了新cryptolepine的作用机制和细胞毒性,它与母体异构体的区别只是吲哚单位相对于喹啉部分的取向。本文的生化和物理化学结果表明,新cryptolepine也插入DNA,优先在GC-rich序列,但与cryptolepine相比,对DNA的亲和力降低。这两种生物碱干扰人拓扑异构酶II的催化活性,但隐tolepine的中毒活性略高于其异构体。这些数据提供了一个分子基础来解释与母体药物相比,新cryptolepine的细胞毒性降低。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
DNA intercalation, topoisomerase II inhibition and cytotoxic activity of the plant alkaloid neocryptolepine.

Cryptolepine and neocryptolepine are two indoloquinoline alkaloids isolated from the roots of the African plant Cryptolepis sanguinolenta. Both drugs have revealed antibacterial and antiparasitic activities and are strongly cytotoxic to tumour cells. We have recently shown that cryptolepine can intercalate into DNA and stimulates DNA cleavage by human topoisomerase II. In this study, we have investigated the mechanism of action and cytotoxicity of neocryptolepine, which differs from the parent isomer only by the orientation of the indole unit with respect to the quinoline moiety. The biochemical and physicochemical results presented here indicate that neocryptolepine also intercalates into DNA, preferentially at GC-rich sequences, but exhibits a reduced affinity for DNA compared with cryptolepine. The two alkaloids interfere with the catalytic activity of human topoisomerase II but the poisoning activity is slightly more pronounced with cryptolepine than with its isomer. The data provide a molecular basis to account for the reduced cytotoxicity of neocryptolepine compared with the parent drug.

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