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HU-331:一种大麻素醌,具有罕见的细胞毒性特性且毒性较低。

HU-331: a cannabinoid quinone, with uncommon cytotoxic properties and low toxicity.

作者信息

Peters Maximilian, Kogan Natalya M

机构信息

The Hebrew University, Department of Medicinal Chemistry and Natural Products, School of Pharmacy, Jerusalem, Israel.

出版信息

Expert Opin Investig Drugs. 2007 Sep;16(9):1405-13. doi: 10.1517/13543784.16.9.1405.

Abstract

The oxidation of cannabis constituents has given rise to their corresponding quinones, which have been identified as cytotoxic agents. Out of these molecules the quinone of cannabidiol--the most abundant non-psychoactive cannabinoid in Cannabis sativa--has shown the highest cytotoxicity. This compound was named HU-331 and it exerts antiangiogenic properties, induces apoptosis to endothelial cells and inhibits topoisomerase II in nanomolar concentrations. Unlike other quinones, it is not cardiotoxic and does not induce the formation of free radicals. A comparative in vivo study in mice has shown HU-331 to be less toxic and more effective than the commonly used doxorubicin. This review summarises the properties of HU-331 and compares it with doxorubicin and other topoisomerase II inhibitors.

摘要

大麻成分的氧化产生了它们相应的醌类物质,这些醌类物质已被鉴定为细胞毒性剂。在这些分子中,大麻二酚(大麻中含量最丰富的非精神活性大麻素)的醌类显示出最高的细胞毒性。这种化合物被命名为HU - 331,它具有抗血管生成特性,能诱导内皮细胞凋亡,并在纳摩尔浓度下抑制拓扑异构酶II。与其他醌类不同,它没有心脏毒性,也不诱导自由基的形成。一项在小鼠身上进行的体内比较研究表明,HU - 331比常用的阿霉素毒性更小、效果更好。这篇综述总结了HU - 331的特性,并将其与阿霉素及其他拓扑异构酶II抑制剂进行了比较。

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