针对 DNA 和 MMP-10/13 的新型肿瘤选择性 s-三嗪的结构优化和分子动力学研究,用于阻止结直肠癌和继发性肝癌的发生。

IF 5.6 2区 医学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY
Christine A Morcos, Nesreen S Haiba, Rafik W Bassily, Marwa M Abu-Serie, Amira F El-Yazbi, Omar A Soliman, Sherine N Khattab, Mohamed Teleb
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引用次数: 0

摘要

合成了一系列具有 DNA 靶向药和非羟胺 MMPs 抑制剂药效学特征的三唑系三嗪类化合物,并通过 MTT 试验对 HCT-116、Caco-2 细胞和正常结肠细胞进行了筛选。7a 和 7g 对 HCT-116 细胞的效力(IC50 = 0.87 和 1.41 nM)和安全性(SI = 181.93 和 54.41)均超过多柔比星。7g 对肝癌(HepG-2;IC50 = 65.08 nM)有特效,肝癌是 CRC 的主要转移部位,与 MMP-13 的表达有关。与多柔比星(DNA 损伤为 0.76 nM,凋亡诱导率为 40.21%)相比,两种衍生物诱导的 DNA 损伤分别为 2.67 nM 和 1.87 nM,破坏了 HCT-116 细胞周期,凋亡诱导率为 33.17%。7g 对 MMP-10(IC50 = 0.205 μM)和 MMP-13(IC50 = 0.275 μM)的作用超过了 NNGH,并将与 CRC 进展相关的 HCT-116 血管内皮生长因子下调了 38%。Docking 和 MD 模拟了配体与受体的结合模式,并强调了 SAR。通过计算预测了它们的 ADMET 特征、药物亲和性和可能的非靶点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Structure optimization and molecular dynamics studies of new tumor-selective s-triazines targeting DNA and MMP-10/13 for halting colorectal and secondary liver cancers.

A series of triazole-tethered triazines bearing pharmacophoric features of DNA-targeting agents and non-hydroxamate MMPs inhibitors were synthesized and screened against HCT-116, Caco-2 cells, and normal colonocytes by MTT assay. 7a and 7g surpassed doxorubicin against HCT-116 cells regarding potency (IC50 = 0.87 and 1.41 nM) and safety (SI = 181.93 and 54.41). 7g was potent against liver cancer (HepG-2; IC50 = 65.08 nM), the main metastatic site of CRC with correlation to MMP-13 expression. Both derivatives induced DNA damage at 2.67 and 1.87 nM, disrupted HCT-116 cell cycle and triggered apoptosis by 33.17% compared to doxorubicin (DNA damage at 0.76 nM and 40.21% apoptosis induction). 7g surpassed NNGH against MMP-10 (IC50 = 0.205 μM) and MMP-13 (IC50 = 0.275 μM) and downregulated HCT-116 VEGF related to CRC progression by 38%. Docking and MDs simulated ligands-receptors binding modes and highlighted SAR. Their ADMET profiles, drug-likeness and possible off-targets were computationally predicted.

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来源期刊
CiteScore
10.30
自引率
10.70%
发文量
195
审稿时长
4-8 weeks
期刊介绍: Journal of Enzyme Inhibition and Medicinal Chemistry publishes open access research on enzyme inhibitors, inhibitory processes, and agonist/antagonist receptor interactions in the development of medicinal and anti-cancer agents. Journal of Enzyme Inhibition and Medicinal Chemistry aims to provide an international and interdisciplinary platform for the latest findings in enzyme inhibition research. The journal’s focus includes current developments in: Enzymology; Cell biology; Chemical biology; Microbiology; Physiology; Pharmacology leading to drug design; Molecular recognition processes; Distribution and metabolism of biologically active compounds.
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