In vitro Evaluation and Molecular Docking Analysis of Potential Anticancer Compounds from Syzygium alternifolium

M. L. Madhuri, R. Reddy
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Abstract

Around the world, Syzygium alternifolium is widely distributed in tropical and subtropical areas. This plant has traditionally been used to treat a variety of illnesses, including cancer. The current research compared the standard drug doxorubicin to the anticancer activity of methanolic extract of Syzygium alternifolium bark on human hepatocyte carcinoma (HepG2) cell line. Through DNA intercalation, inhibition of topoisomerase-II-mediated DNA repair, free radical production and consequent damage to cellular membranes, DNA, and proteins, doxorubicin exerts its anticancer activity in cancerous cells. Research on cytotoxicity have shown that Syzygium alternifolium phytoconstituents can selectively target cancer cells (IC50 = 185.585 µg/ml), while having little to no cytotoxic effects on normal cells Using Mcule docking software, molecular docking studies were performed against the human Topoisomerase-2 and CDK-2 proteins (Protein Data Bank-ID: 1ZXM and 1DI8, respectively). Seven compounds from the bioactives isolated are considered as safe inhibitors, according to in silico studies. In order to better understand the probable mechanisms of action and create more efficient and cost-effective therapies, molecular docking experiments were carried out employing phytoconstituents. This study demonstrates a significant consistency of anticancer therapeutic drug potentials of Syzygium alternifolium by in vitro and in silico approaches, leading the way for a better understanding of how integrating molecular docking and in vitro studies can improve the identification of cancer drugs.
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互花合欢潜在抗癌化合物的体外评价及分子对接分析
在世界范围内,互花合欢广泛分布于热带和亚热带地区。传统上,这种植物被用来治疗包括癌症在内的各种疾病。本研究比较了标准药物多柔比星与合藤树皮甲醇提取物对人肝癌(HepG2)细胞系的抗癌活性。阿霉素通过插入DNA、抑制拓扑异构酶ii介导的DNA修复、自由基的产生以及随后对细胞膜、DNA和蛋白质的损伤,在癌细胞中发挥其抗癌活性。细胞毒性研究表明,互花合子植物成分可以选择性靶向癌细胞(IC50 = 185.585µg/ml),而对正常细胞几乎没有细胞毒性作用。利用Mcule对接软件,对人类拓扑异构酶-2和CDK-2蛋白(Protein Data Bank-ID: 1ZXM和1DI8)进行了分子对接研究。根据计算机研究,从生物活性物质中分离出的7种化合物被认为是安全的抑制剂。为了更好地了解其可能的作用机制,并创造更有效和更具成本效益的治疗方法,采用植物成分进行了分子对接实验。本研究通过体外和计算机方法证明了互花合欢的抗癌治疗药物潜力具有显著的一致性,为更好地理解如何将分子对接和体外研究结合起来提高癌症药物的鉴定提供了途径。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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