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首页> 外文期刊>Bioorganic and Medicinal Chemistry >Tri-, tetra- and heptacyclic perylene analogues as new potential antineoplastic agents based on DNA telomerase inhibition
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Tri-, tetra- and heptacyclic perylene analogues as new potential antineoplastic agents based on DNA telomerase inhibition

机译:三环,四环和七环per类似物作为基于DNA端粒酶抑制作用的新型潜在抗肿瘤药

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摘要

A recent approach in anticancer chemotherapy envisages telomerase as a potentially useful target. An attractive strategy deals with the development of compounds able to stabilize telomeric DNA in the G-quadruplex folded structure and, among them, a prominent position is found in the perylenes. With the aim to further investigate the role of drug structure, in view of possible pharmaceutical applications, we synthesized a series of compounds related to PIPER, a well-known perylene-based telomerase inhibitor. We modified the number of condensed aromatic rings and introduced different side chains to modulate drug protonation state and extent of self-aggregation. Effective telomerase inhibition was induced by heptacyclic analogues only, some showing a remarkably wide selectivity index with reference to inhibition of Taq polymerase. G-quadruplex stabilization was monitored by circular dichro-ism and melting experiments. Cell cytotoxicity measurements indicated a poor short-term cell killing ability for the best G-quartet binders. Besides the presence of a planar seven-condensed ring system, the introduction of a cyclic amine in the side chains critically affects the selectivity window.
机译:抗癌化学疗法的最新方法设想端粒酶可能是有用的靶标。一种有吸引力的策略涉及能够稳定G-四链体折叠结构中端粒DNA的化合物的开发,其中,在per中发现重要位置。为了进一步研究药物结构的作用,鉴于可能的药物应用,我们合成了一系列与PIPER有关的化合物,PIPER是一种众所周知的per基端粒酶抑制剂。我们修改了稠合的芳环的数量,并引入了不同的侧链来调节药物的质子化状态和自聚集程度。端粒酶的有效抑制仅是由七环类似物诱导的,相对于Taq聚合酶的抑制,有些具有明显的选择性指数。通过圆二色性和熔融实验监测G-四链体的稳定性。细胞毒性测定表明,最佳G四联体结合剂的短期细胞杀伤能力较差。除了存在平面七缩环系统外,在侧链中引入环胺还会严重影响选择性窗口。

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