Fortin Sébastien, Moreau Emmanuel, Patenaude Alexandre, Desjardins Michel, Lacroix Jacques, Rousseau Jean L C, C-Gaudreault René
Unité des Biotechnologies et de Bioingénierie, Centre de Recherche, C.H.U.Q., Hôpital Saint-François d'Assise, Université Laval, Québec, QC, Canada G01L 3L5.
Bioorg Med Chem. 2007 Feb 1;15(3):1430-8. doi: 10.1016/j.bmc.2006.11.005. Epub 2006 Nov 10.
Tubulin is the target of many anticancer drugs, including N-phenyl-N'-(2-chloroethyl)urea (CEU). Unlike most anti-beta-tubulin agents, CEUs are protein monoalkylating agents binding through their N'-(2-chloroethyl)urea moiety to an amino acid nearby the colchicine-binding site on beta-tubulin isoform-2. Following the previously synthesized and attractive N-(3-omega-hydroxyalkylphenyl)-N'-(2-chloroethyl)urea that exhibited growth inhibitory activity at the nanomolar level, we investigated the importance of lower alkyl and alkoxy groups to evaluate the effect of hydroxylated group and chain length on both cell growth inhibition and the mechanism of action of CEU. Here, we describe the preparation of two new series of CEU and show that the most potent CEU derivatives beside the omega-hydroxylated 1f were 2f and 3e, respectively. We have confirmed that the pentyl substituted CEUs 1f, 2f, and 3e are still covalently binding to beta-tubulin and still arrest cell division in G(2)/M phase.
微管蛋白是许多抗癌药物的作用靶点,包括N-苯基-N'-(2-氯乙基)脲(CEU)。与大多数抗β-微管蛋白药物不同,CEU是蛋白质单烷基化剂,通过其N'-(2-氯乙基)脲部分与β-微管蛋白同工型2上秋水仙碱结合位点附近的一个氨基酸结合。继先前合成的具有纳摩尔水平生长抑制活性的有吸引力的N-(3-ω-羟烷基苯基)-N'-(2-氯乙基)脲之后,我们研究了低级烷基和烷氧基的重要性,以评估羟基化基团和链长度对细胞生长抑制及CEU作用机制的影响。在此,我们描述了两个新系列CEU的制备,并表明除了ω-羟基化的1f之外,最有效的CEU衍生物分别是2f和3e。我们已经证实,戊基取代的CEU 1f、2f和3e仍然与β-微管蛋白共价结合,并且仍然使细胞分裂停滞在G(2)/M期。
Zotero 插件