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N-环取代苯并芘 G-四链体配体系列中的芳核扩展:增加端粒损伤、抗肿瘤活性,并对肿瘤细胞有很强的选择性,而对健康细胞的选择性较弱。

Aromatic core extension in the series of N-cyclic bay-substituted perylene G-quadruplex ligands: increased telomere damage, antitumor activity, and strong selectivity for neoplastic over healthy cells.

机构信息

Dipartimento di Chimica, Sapienza Università di Roma, P.le.A. Moro 5, 00185 Roma, Italy.

出版信息

ChemMedChem. 2012 Dec;7(12):2144-54. doi: 10.1002/cmdc.201200348. Epub 2012 Oct 24.

DOI:10.1002/cmdc.201200348
PMID:23097341
Abstract

Based on previous work on both perylene and coronene derivatives as G-quadruplex binders, a novel chimeric compound was designed: N,N'-bis[2-(1-piperidino)-ethyl]-1-(1-piperidinyl)-6-[2-(1-piperidino)-ethyl]-benzo[ghi]perylene-3,4:9,10-tetracarboxylic diimide (EMICORON), having one piperidinyl group bound to the perylene bay area (positions 1, 12 and 6, 7 of the aromatic core), sufficient to guarantee good selectivity, and an extended aromatic core able to increase the stacking interactions with the terminal tetrad of the G-quadruplex. The obtained "chimera" molecule, EMICORON, rapidly triggers extensive DNA damage of telomeres, associated with the delocalization of telomeric protein protection of telomeres 1 (POT1), and efficiently limits the growth of both telomerase-positive and -negative tumor cells. Notably, the biological effects of EMICORON are more potent than those of the previously described perylene derivative (PPL3C), and more interestingly, EMICORON appears to be detrimental to transformed and tumor cells, while normal fibroblasts expressing telomerase remain unaffected. These results identify a new promising G-quadruplex ligand, structurally and biologically similar on one side to coronene and on the other side to a bay-monosubstituted perylene, that warrants further studies.

摘要

基于先前对苝和蒄衍生物作为 G-四链体结合物的研究,设计了一种新型的杂化化合物:N,N'-双[2-(1-哌啶基)-乙基]-1-(1-哌啶基)-6-[2-(1-哌啶基)-乙基]-苯并[ghi]苝-3,4:9,10-四羧酸二酰亚胺(EMICORON),其中一个哌啶基结合在苝的海湾区域(芳香核的 1、12 和 6、7 位),足以保证良好的选择性,并且扩展的芳香核能够增加与 G-四链体末端四联体的堆积相互作用。所得的“嵌合体”分子 EMICORON 可迅速引发端粒的广泛 DNA 损伤,伴随着端粒蛋白保护端粒 1(POT1)的离域,并且有效地限制了端粒酶阳性和阴性肿瘤细胞的生长。值得注意的是,EMICORON 的生物学效应比先前描述的苝衍生物(PPL3C)更有效,更有趣的是,EMICORON 似乎对转化和肿瘤细胞有害,而表达端粒酶的正常成纤维细胞则不受影响。这些结果确定了一种新的有前途的 G-四链体配体,在结构和生物学上与蒄相似,另一方面与苯并[ghi]苝的海湾单取代物相似,值得进一步研究。

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