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Detailed investigation of anticancer activity of sulfamoyl benz(sulfon) amides and 1H-pyrazol-4-yl benzamides: An experimental and computational study

机译:磺酰苯甲酰苯锆(磺酰苯甲锌酰胺和1H-吡唑-4-基苯甲酰苯胺的详细研究:实验和计算研究

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摘要

Cancer is the second leading cause of mortality worldwide. Therapeutic approach to cancer is a multi-faceted one, whereby many cellular/enzymatic pathways have been discovered as important drug targets for the treatment of cancer. A major disadvantage of most of the currently available anticancer drugs is their non-selective cytotoxicity towards cancerous as well as healthy cells. Another major hurdle in cancer therapy is the development of resistance to anticancer drugs. This necessitates the discovery of new molecules with potent and selective cytotoxic activity towards only cancerous cells, with minimum or no damage to the normal/healthy cells. Herein we report detailed investigation into the anticancer activity of sulfamoyl benz(sulfon)amides (1a-1g, 2a-2k) and 1H-pyrazol-4-yl benzamides (3a-3j) against three cancer cell lines, breast cancer cells (MCF-7), bone-marrow cancer cells (K-562) and cervical cancer cells (HeLa). For comparison, screening against healthy baby hamster kidney cells (BHK-21) was carried out. All compounds exhibited selective cytotoxicity towards cancerous cells. Cell cycle analysis was carried out using flow cytometry, followed by fluorescence microscopic analysis. DNA interaction and docking studies were also carried out.
机译:癌症是全世界死亡的第二大原因。治疗方法癌症是一个多面的一个,因此许多蜂窝/酶途径已发现的重要药物靶点治疗癌症。大部分目前可用的抗癌药的主要缺点是它们对癌细胞的非选择性细胞毒性以及健康的细胞。在癌症治疗的主要障碍是耐药的发展抗癌药物。这需要新分子与有效的和选择性的细胞毒活性的发现向仅癌细胞,以最小的或到正常/健康细胞没有损伤。本文我们报告详细调查氨磺酰苯并(砜)酰胺(1A-1G,2A-2K)和1H-吡唑-4-基苯甲酰胺(图3a-3j中)针对3种癌细胞系,乳房癌细胞的抗癌活性(MCF -7),骨髓癌细胞(K-562)和宫颈癌细胞(HeLa细胞)。为了便于比较,筛选对健康的幼仓鼠肾细胞(BHK-21)进行。所有化合物显示出选择性细胞毒性对癌细胞。细胞周期分析进行了使用流式细胞术,随后用荧光显微镜分析。 DNA的相互作用和对接的研究也进行了。

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